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  1. Jul 2018
    1. On 2017 Jul 14, Randi Pechacek commented:

      Marcus Leung, first author of this paper, gave some background on a microBEnet blog post.


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    1. On 2015 Apr 08, DOMINIQUE BERGMANN commented:

      An anonymous peer noted that panels 6D-E are identical. This is an error on our part and we have identified the source of the error and the raw data that corresponds to the genotypes pictured. Table 2 contains quantified data related to the information in panel 6D-E and is correct. All conclusions in the paper are based on the data in Table 2. We are working to correct this error with the journal.


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    1. On 2014 Sep 02, Haoquan Wu commented:

      Around 7 years ago, we have shown an extensive degree of heterogeneity at the end of mature miRNA, which can affect detection by real-time PCR employing stem-loop primer mediated RT-PCR.

      http://www.plosone.org/article/info:doi/10.1371/journal.pone.0001020


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    1. On 2015 Feb 06, Pavel Baranov commented:

      This paper provides an invaluable dataset of context dependent translation initiation start (TIS) efficiency. While the optimal (Kozak) TIS context has been determined a long time ago, estimating the power of individual TIS based on the contexts was usually qualitative, at best it was based on position weight matrices where the weight of each individual nucleotide was taken into account independently of other nucleotides. By systematically randomizing the context surrounding AUG codons Noderer et al measured TIS efficiencies of all 11-mers containing AUG codons. The dataset is available in Supplementary Table 2.


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    1. On 2014 Oct 03, Friedrich Thinnes commented:

      To finalize three-dimensional VDAC structure: Focus on Native VDAC will be indispensable

      This study, from my point of view, marks a great moment of VDAC research:

      1) It points another time to the relevance of cell membrane-standing VDAC-1 for the pathogenesis of Alzheimer´s Disease via apoptosis.

      2) It gives strong support to the cell membrane-expression, more precisely plasmalemmal lipid raft-integration of vertebrate VDAC-1. Furthermore, the data concerning the posphorylation of VDAC-1 in correlation to regulation of channel opening/closing argue in favor of its involvement in cell volume regulation and thus apoptosis. They are in line with much evidence indicating that plasmalemmal VDAC-1 forms the channel part of a volume regulated anion channel complex (VRAC/VSOAC).

      3) From here, VDAC-1 in the plasmalemma must be “fully closed” = collapsed = N-terminus accessible outside the barrel = closed for anions and cations, and there is evidence that the N-terminal part of native VDAC-1 can be reached by antibodies even in detergent solutions (Benz et al., 1992; Thinnes and Burckhardt, 2012).

      4) Applying canonical incorporation into black membranes, detergent-solubilized native phosphorylated mammalian VDAC-1 as well as recombinant channel preparations from E. coli inclusion bodies show only “open” = anion-selective = N-terminal stretch inside the barrel and “closed” = cation-selective = semi-collapsed = N-terminal stretch inside the barrel channel phenotypes (Teijido et al., 2012). “Fully closed” = collapsed = N-terminus accessible outside the barrel VDAC-1 states thus cannot be studied by this approach. The same holds true for more recent crystallization-based approaches. However, upcoming laser-based approaches may work just on native VDAC-1 in solutions; thus improvements to get detergent solubilized native VDAC preparation may pay to keep on the schedule.

      --Benz R, Maier E, Thinnes FP, Götz H, Hilschmann N (1992) Studies on human porin. VII. The channel properties of the human B-lymphocyte membrane-derived “Porin 31HL” are similar to those of mitochondrial porins, Biol. Chem. Hoppe Seyler. 373: 295–303. --Thinnes FP, Burckhardt G (2012) On a fully closed state of native human type-1 VDAC enriched in Nonidet P40. Mol Genet Metab 107: 632-633. --Teijido O, Ujwal R, Hillerdal CO, Kullman L, Rostovtseva TK, Abramson J (2012) Affixing N-terminal α-helix to the wall of the voltage-dependent anion channel does not prevent its voltage gating. J Biol Chem 287: 11437-11445.


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    1. On 2015 Aug 14, Oliver T Mytton commented:

      We note the comments for Kaiser et al. We are in the process of compiling a full response. When this is ready we will post it on the BMC Public Health website, linked directly to the article.

      Oliver Mytton Honorary Specialty Registrar, Centre for Diet and Activity Research (CEDAR), MRC Epidemiology Unit, Cambridge.


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    2. On 2015 Jul 08, Kathryn Kaiser commented:

      Having recently published a paper on the same topic [1], we read this paper (published August, 2014) by Mytton and colleagues (the authors) with great interest. We identified several important issues that vitiate confidence in the paper by the authors [2].

      Errors of calculation, stated protocol violations, and documentation:

      Our first concern pertains to differences in calculations in a study we both included, as well as the irreproducibility of the standard errors (SEs) reported in the Figure 2a forest plot of effects on body weight in [2]. First, we believe there is a calculation error in how the authors derived the effect size and variance in [2] for Whybrow, 2006 [3], which we both included. For clarity, we note the correct citation for the Whybrow paper is 2006, though it is sometimes cited as 2007 in [2]. Per [4], in order to reduce the potential for the over influence of studies where there are two experimental groups (300 grams per day and 600 grams per day in the case of Whybrow, 2006 [3]) compared to only a single control group, the control number (in this case, n=14) should be divided in half and rounded if necessary to the nearest integer for meta-analysis. We both calculated the same mean differences (ours reported as standardized mean differences), but substantially different confidence intervals. In the original report of outcomes [3], the effects on body weight for both treatment groups were not significant, whereas in Figure 2a [2], the confidence intervals are represented as showing a statistically significant effect for both treatment groups.

      After further examination of standard errors for the other studies in included by the authors, and being unable to recreate several of the values reported in the paper [2], we recomputed the meta-analytic statistics from the source papers after making corrections to these values (see list below for all corrected estimates). For the overall analysis, this resulted in a smaller effect [-0.54 (-1.05,-0.03)] than reported in [2]. In a more appropriate analysis and using corrected standard errors, we removed an outlier [5] that the authors had identified in the “Comparison with other studies” section on page 9 of [2]. This study had a drop-out rate of over 52 percent, did not conduct an intent-to-treat analysis, and included only 9 subjects in the final analysis. When removing this paper as suggested in [2] (but not done in Figure 2), the overall effect is -0.31 (-0.70, 0.07), p=0.11, with a drop in heterogeneity from 72 to 53%.

      Recalculated forest plot of included studies, excluding [5] are as follows (Mean Difference in Kg, 95% Confidence Interval, Standard Error): Smith-Warner 2000: (-0.09, -0.40 to 0.22, 0.16); Whybrow 2006 (600g group): (-0.62, -1.52 to 0.28, 0.46); Whybrow 2006 (300g group): (-0.77, -1.73 to 0.19, 0.49); Basu 2010: (-0.90, -1.88 to 0.08, 0.50); Peterson 2011: (0.40, -0.05 to 0.85, 0.23); Dow 2012: (-0.50, -1.30 to 0.30, 0.41); Christensen 2013: (-0.90, -2.17 to 0.37, 0.65).

      Concerning study inclusion based on the stated protocol, the authors were not consistent in the application of their criteria. The authors opted to include one study of individuals with newly diagnosed diabetes [6], despite their exclusion criterion of studies with “subjects with a medical illness that was liable to lead to weight loss or weight gain.”[2] Excluding only this study also results in non-significant findings [excluding [6]: -0.51 (-1.06, 0.03); excluding both the outlier [5] and [6] results in: -0.27 (-0.67, 0.13)]. In other words, correcting the apparent errors of inclusion and effect size calculations changes the conclusions as stated in the paper [2].

      Other points of note:

      Although some differences between our papers are the result of simple methodological differences, such as our limitation to longer than eight week studies versus the authors limitation to four weeks, other differences are more substantial. We note that the authors [2] did not use the term “obesity” in their list of keywords, which is an important omission in a review looking at weight outcomes. In addition, the authors included three studies that investigated changes in only a single fruit or vegetable, while we opted to include studies where the intervention was a variety of fruits and vegetables, in order to evaluate the more general public health message that is common today. This difference in inclusion simply represents a nuanced difference between our analyses, but it is important that searches are designed to adequately answer the question at hand. For instance, in applying the stated criteria given by the authors, we found three examples [7-9] of other studies of a single fruit or vegetable that were not included by the authors but appear to meet criteria, calling into question the thoroughness of the literature search.

      Lastly, in trying to reproduce the authors work, we noted that the list of included studies in Table 1 includes Singh, 1992 [10] while the final analysis does not. The reviewer comments and author replies posted on line at the BMC Public Health journal website indicate the authors followed the reviewer recommendation to remove the Singh paper from the analysis, yet it remains in the published table and appears to also be counted in the number in the PRISMA diagram, Figure 1. According to the forest plots in Figure 2, 7 studies were included for weight outcomes and 5 studies were included for energy intake outcomes. Figure 1 does not match the included studies in the search results reported.

      Conclusion:

      It is clear that the report presented by the authors has several concerning errors, is not consistent within itself, and does not support the conclusion the paper states that these interventions, “…result in either a small reduction in body weight or reduced weight gain relative to controls.”[2] We respectfully request that the authors reply to these concerns in order to correct the record.

      Kathryn A. Kaiser, Ph.D. Andrew W. Brown, Ph.D. David B. Allison, Ph.D. Office of Energetics, Nutrition and Obesity Research Center, School of Public Health, University of Alabama at Birmingham

      References

      \1.\ Kaiser KA, 2014 \2.\ Mytton OT, 2014 \3.\ Whybrow S, 2006 \4.\ http://handbook.cochrane.org/ \5.\ Weerts SE, 2011 \6.\ Christensen AS, 2013 \7.\ Lehtonen HM, 2010 \8.\ Thies F, 2012 \9.\ Vafa MR, 2011 \10.\ Singh RB, 1992


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    1. On 2014 Oct 21, Paula Rahal commented:

      Acknowledgements

      We thank Dr. Daniel Seabra and Dr. Eliney Ferreira Faria for their collaboration in collecting the samples and Dr. Ligia Maria Kerr for pathological review. This work was supported by São Paulo State Research Foundation - FAPESP (2010/01661-2) and CNPq.


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    1. On 2015 Nov 13, Lydia Maniatis commented:

      The theory and method of this study simply doesn't hold up to scrutiny. Very serious problems include:

      Methods

      1. The authors claim to be motivated by previous findings of “large individual differences in lightness constancy with respect to changes in surface slant...” Yet they have only two observers per condition, and one of the observers did not complete all of the replications. Large individual differences are an indication that stimuli are ambiguous to observers, who consequently have to make quasi-guesses. In this type of situation there tends to be both intra- and inter-individual variability. Here, the small number of observers does not make either form of variability detectable.

      2. They describe having subjected observers to an “induction procedure (Allred & Brainard, 2009; Doerschner, Boyaci & Maloney, 2004) to familiarize them with the difference between surface reflectance...and the amount of light reflected from a surface [luminance]...” Surface reflectance is not perceived, but inferred (the perceptual correlate is lightness), and luminance has no perceptual correlate. The relative luminances of surfaces in context and their geometrical relationships conspire to produce local impressions of both lightness and apparent illumination. You cannot train observers to perceive luminance, which, again has no perceptual correlate (it does not correspond to white, gray, black; virtually any luminance can take on any of these perceptual values).

      An example can help make clear why such a “induction procedure” is theoretically and methodologically hollow. This is the video version of the Adelson checkerboard illusion, in which we see a square being moved from apparent shadow to apparent plain view, and changing apparent color. We can watch the video over and over again without thereby learning to see the square as constant in both its luminance and its reflectance.

      1. Asking subjects to rate the similarity in lightness of surfaces on a scale of 1 to 30 seems quite unrealistic.

      2. The mathematical acrobatics necessitated by the general shoddiness and ambiguity of the methods are moot.

      Theory

      The authors state that “Changing the orientation of an object's surface with respect to a directional light source affects the luminance of the reflected light [they mean "the luminance of the surface"] even when the light emitted by the illumination sources is held constant.” That's true.

      However, the next statement is incomplete and misleading: “The visual system can stabilize lightness with respect to such geometrical effects...” This statement needs to be highly qualified. The visual system can achieve such “lightness constancy” (requiring disambiguation of reflectance and illumination) only if the image conditions support it. An isolated surface (as that used by the authors), whether fronto-parallel or slanted, will not offer much or any such support. Thus, it should not be surprising that the authors found "essentially no lightness constancy with respect to changing the slant of a test surface..." and that "the dissimilarity data were well-accounted for by a one-dimensional perceptual representation..."

      While, again, this outcome was highly predictable, they authors are mystified by it. Noting that their results differ from those of Logvinenko and Maloney (2006), they confess that "We do not know the reason for this difference." But as they note, in that study the illumination differences were not only actual, they were (more importantly) APPARENT (a fact that can be ascertained on the basis of observation), because the setting was less spare and more informative. This is something that should have been considered before, not after data collection.

      But lightness facts and relevant literature are not of interest to these authors, who dispense with the matter early on, saying: “This form of lightness constancy [the slant surface form?] is not well-understood.” And on to data collection.


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    1. On 2014 Oct 06, Leonid Teytelman commented:

      Dear Authors,

      We have published an analysis in S. cerevisiae, showing expression-dependent artifactual ChIP enrichment at highly expressed loci (Teytelman L, 2013 "Highly expressed loci are vulnerable to misleading ChIP localization of multiple unrelated proteins"). As you know, our finding raises the question of whether HOT regions may also be influenced by the same artifact.

      It is great that you have considered our work and have thoughtfully responded to our analysis. Below, I would like to continue this discussion in an effort to better understand the artifact, its causes, and whether it may be contributing to the enrichment at the HOT loci.

      1. “we have demonstrated that there is no correlation between our non-specific binding controls (IgG) and our measured transcription factor occupancy;”

      Considering our results with no-tag control experiments, an IgG may fail to control for the artifact. It would be great if you could instead perform a GFP ChIP-Seq, similarly to what we have done in yeast.

      2. The regions determined in ref. 41 have very low enrichment (twofold or less) of non-specific immunoprecipation in anti-GFP antibody controls over input DNA evaluated using a non-standard sliding-window approach. Importantly, immunoprecipitation/input ratios at this level are typically not considered enriched for binding in modern peak-calling procedures. For example, the median immunoprecipitation/input ratio for our human RNA Pol II experiments is 20-fold, and only 0.033% of human RNA Pol II peaks contain an immunoprecipitation/input ratio ≤ twofold.

      The mean is low, but in both anti-GFP experiments, there are loci with 3-5x enrichment (figure 4D). Most importantly, while the anti-GFP enrichment at the hyper-ChIPable loci is low, please note that the level of enrichment is variable from protein to protein (2-5X for Sir proteins, but often >10X for Cse4).

      3. Thus, it is essential to note that the term ‘hyper-ChIPable’, coined by ref. 41, is quite misleading, as a correctly performed ChIP experiment will evaluate statistically enriched regions, with higher immunoprecipitation/input ratios. The so-called hyper-ChIPable regions in ref. 41 are not binding regions as determined under ChIP-seq best practices. Hence, when statistical peak-calling was performed in ref. 41 (using the established MACS peak-caller) to evaluate signals only at significantly enriched regions (Supplementary Table 1) only 17 (<7.5%) of the 238 claimed ‘hyper-ChIPable’ regions were called significant by all three Sir proteins. In fact, 68% of their 238 regions do not contain a binding site for any Sir protein as determined by MACS, despite even very liberal settings used (P < 10−5, no fold enrichment cut-off). Thus, the data of ref. 41 contradict its own major claim that all three Sir proteins showed enrichment at the 238 sites.

      By reporting the 238 sites with >2fold enrichment of Sir2, Sir3, and Sir4, we are in fact being extra-demanding in terms of the threshold. We are stringently requiring all three proteins to be enriched above a threshold at the locus. So a target with 5x enrichment of Sir2 and 1.8X enrichment of Sir3 would not pass this cutoff. A typical ChIP study will focus on a single factor at a time. Had we done that, we would have many more artifactual targets for each silencing protein, with many at 5x or higher enrichment. Furthermore, the level of the artifactual signal varies from protein to protein or experiment to experiment. For example, the Cse4 signal at highly-expressed loci can give 10x or higher enrichment.

      4. Furthermore, as indicated in Supplementary Table 3 of ref. 41, the Sir2, Sir3 and Sir4 ChIP-seq experiments were performed only once each, which raises the question as to whether enrichment of Sir proteins at the 238 sites is reproducible. More rigorously, even for the remaining 17 genomic loci, their status as hyper-ChIPable is questionable as each region would first have to be established as a reproducible binding site in replicate experiments for each individual Sir protein. If you consider that Sir2, Sir3 and Sir4 ChIP-seq constitutes three replicates of Sir proteins, their data show that most of their claimed sites were not reproducibly enriched.

      Most of our artifact-cause analysis focuses on genome-wide data, not on the 238 sites. The 238 Sir-enriched euchromatic loci were a launching point for the analysis, but most of the paper looks comprehensively at the link between expression and ChIP levels. Figures 3, 4, and 5 are all on genome-wide correlations between Pol II/III and ChIP.

      As for reproducibility, we see the same peaks, with often 10x enrichment, in Ste12, Cse4, two distinct GFP experiments, and each of the three Sir ChIP-Seq datasets. The same exact loci come up in the Sir3 paper from Oliver Rando’s group (Radman-Livaja M, 2011).

      5. In addition to the analytical differences outlined above, other potential sources for the marked differences between our data and the Sir-enriched regions of ref. 41 are deviations from a typical ChIP protocol. In particular, ref. 41 employed a significantly longer cross-link time (1 h as opposed to the typical 10–20 min). This might contribute to formation of large non-specific protein–DNA complexes, which can in turn increase non-specific immunoprecipitation.

      Though not discussed in the manuscript, we have in fact performed experiments to investigate if the crosslinking concentration contributed to the misleading signal. We performed ChIP with the 1 hour crosslinking at room temperature at the following formaldehyde concentrations: 0.0625%, .125%, .25%, .5% and 1%, but did not find a proportionate decrease in the hyper ChIPpable signal with the decreasing formaldehyde concentrations. Moreover, the presence of hyper-ChIPability in the Snyder datasets (Cse4, Ste12), ours (Sir2, 3, 4, GFP), and Rando (Sir3) make it clear that the problem is not in some unusual protocol steps in our hands.

      We also note that we initially performed the Sir ChIP-Seq experiments because of our interest in the Sir protein biology. Because the Sir proteins do not directly interact with the DNA, we used longer crosslinking times. This is not unique to our work.


      In summary, much more work is needed to pinpoint the cause of the artifact and to evaluate whether some or all of the signal at highly expressed genes in many other reported ChIP studies could be artifactual. Much more work is necessary to develop the best controls and corrections for the artifact. However, the artifact we report is not minor and is not a consequence of the methodological details of our manuscript.

      Also, please note the following papers, published almost in parallel with ours, on this topic:

      Park D, 2013 "Widespread Misinterpretable ChIP-seq Bias in Yeast" (Different analysis methods but the same conclusions in S. cerevisiae, analyzing an entirely different set of factors with ChIP-Seq experiments.)

      Kasinathan S, 2014 "High-resolution mapping of transcription factor binding sites on native chromatin" (Questions specificity of standard ChIP in S. cerevisiae and at HOT regions of Drosophila. This work possibly provides a solution to the artifact with a modification of the ChIP technique.)

      Also, the following discussion of our work on PubPeer may be useful.


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    1. On 2014 Oct 14, Hilda Bastian commented:

      Thanks for drawing attention to this interesting article. Dancer SJ, 2009 argued that what's done now in an outbreak is "a veritable blunderbuss approach." Dancer's own cross-over study of enhanced cleaning addressed MRSA, although the study was too small to identify a definite impact on infection (Dancer SJ, 2009).

      Environmental strategies were included in a systematic review of measures to reduce the spread of VRE (with a search for evidence up to June 2012)(De Angelis G, 2014). De Angelis found only two studies, concluding that no definite impact on infection had been identified (Hayden MK, 2006; Williams VR, 2009).

      This new retrospective study (Everett BR, 2017) seems to be the second looking at the implementation of this particular set of strategies. The first was undertaken by the team that developed the method and run the associated consultancy service (Watson PA, 2012).

      Both routinely and during outbreaks, Dancer SJ, 2009 concluded, "there is a lot of work still to do to establish cleaning as an evidence-based science." That still seems to be the case.


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    2. On 2014 Oct 10, Paul Watson commented:

      This is an excellent article showing a simple way to dramatically lower all hospital acquired infections with single cleaning algorithm from Steiros. The final infection rates are extremely low with immediate cost savings that I have not seen with any other infection control process. As a surgeon and an infection control practitioner, I am especially excited about the zero infection rate for total knee arthroplasties in this paper. This is something that we all strive for and has been achieved by few. Thanks for the article.


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    1. On 2014 Sep 30, Ryan Radecki commented:

      Post-publication commentary:

      "Emergency PCI for STEMI is Dead?"

      This somewhat befuddling study tries desperately to create a problem where there probably truly wasn’t – but as soon as the conflict-of-interest disclosures come up, it’s clear why.

      This is the 1-year outcomes from STREAM, a prospective, open-label, parallel-group trial enrolling participants with acute STEMI, but unlikely to undergo primary PCI within 1 hour of diagnosis. Participants were then randomized to either still undergo emergency PCI, or to fibrinolysis followed by urgent or emergency rescue PCI. The initial 1-month composite outcome, despite an excess of deaths secondary to intracranial hemorrhage in the fibrinolysis group, did not demonstrate any disadvantage to fibrinolysis with delayed PCI. There was actually a 2% absolute decrease in the composite outcome favoring fibrinolysis – and thus the 1-year follow-up, hoping this small advantage in morbidity would translate into a measurable mortality advantage....

      http://www.emlitofnote.com/2014/09/emergency-pci-for-stemi-is-dead.html


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    1. On 2014 Sep 10, Vojtech Huser commented:

      Data on how often patients use infobutton (when they login to PHR) is a very valuable contribution.


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    1. On 2017 May 17, Mihai Paduraru commented:

      In relation to this article I published a Critical observation, due to the too many similarities to a randomized controlled trial by Wang et al.: https://doi.org/10.1016/j.ijsu.2017.01.019 (http://www.sciencedirect.com/science/article/pii/S1743919117300201)


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    1. On 2017 Jul 14, Randi Pechacek commented:

      Nicholas Osborne and Richard Sharpe, co-authors of this paper, wrote a joint guest blog post on microBEnet explaining the interesting background for this paper.


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    1. On 2014 Aug 27, Daniel Kripke commented:

      Despite much useful material, the report of Owens and colleagues about insufficient sleep was marred by insufficient evidence-based definition of insufficient sleep. “Sufficient sleep” was “defined as ≥8 hours,” but why? Consider that in a Japanese nation-wide sample of adolescents grade 7 through 12, ≥7-<8 hours was associated with the best General Health in a number of grade groups of boys and girls and overall ≥8-<9 hours was not significantly superior in predicting mental health [1]. Consider that in a unique lifetime study of mortality risk, girls sleeping 2 hours less than the average for age 16 had the same mortality as those sleeping the average, whereas mortality was about the same for boys sleeping 1 hour less than the average [2]. More evidence concerning optimal sleep durations for adolescents is needed. Should we recognize that much of the evidence-absent advocacy for children to sleep more has been financed by hypnotics manufacturers, and has been accompanied by a sharp increase in hypnotic prescriptions for children? 1. Kaneita Y, et al. J Clin Psychiatry 2007;68:1426-1435. 2. Duggan KA, et al. Health Psychol 2014, in press.


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    1. On 2014 Sep 23, Samir Ounzain commented:

      Very nice editorial describing this work by Patrick Hofmann and Reinier Boon can be found here;

      Hofmann P, Boon RA. Non-coding RNA enhances cardiac development. J Mol Cell Cardiol. 2014 Sep 18. pii: S0022-2828(14)00286-7. doi: 10.1016/j.yjmcc.2014.09.005. [Epub ahead of print] PubMed PMID: 25240640.


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    1. On 2015 Mar 18, Airton Stein commented:

      This article is not my publication - Airton Tetelbom Stein from Brazil


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    1. On 2016 Oct 24, Sean Ekins commented:

      Some more recent slides on other social media tools and also using twitter for collaborations in science http://www.slideshare.net/ekinssean/pros-and-cons-of-social-networking-for-scientists


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    2. On 2014 Dec 17, Sean Ekins commented:

      Some slides to expand on this are here http://www.slideshare.net/ekinssean/beyond-the-10-simple-rules


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    3. On 2014 Dec 15, Sean Ekins commented:

      Also added to summary of our 2014 papers http://www.collabchem.com/2014/12/15/a-year-in-publications-2014/


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    4. On 2014 Dec 02, Sean Ekins commented:

      paper mentioned here http://www.collabchem.com/2014/08/25/plos-paper-going-viral/ and here http://www.collabchem.com/2014/08/21/anatomy-of-a-plos-computational-biology-paper/


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    1. On 2014 Aug 22, Gözde Ozakinci commented:

      I have to say - I wish it was clear where the study was done in the abstract.


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    1. On 2017 Oct 01, Misha Koksharov commented:

      Of interest, depletion of an individual MRTF isoform (either MRTF-A or MRTF-B) almost completely suppressed induction of several contractile proteins despite the presence of the other MRTF isoform. This most likely indicates that both isoforms cooperate in expressional up-regulation of contractile proteins and that a certain threshold concentration of MRTF is required in order to stimulate the EMyT.

      During my previous postdoc I've observed similar effects of silencing MRTF-A and MRTF-B separately in U2OS cells when using bioluminescent real-time reporters ("SRF-luciferase") as an output. Before me it was also noticed by Gerber et al, 2013: Fig. 4. We have used the same siRNA SmartPools from Dharmacon: (siRNA sequences are in the links) against human MRTF-A, MRTF-B and SRF (and in some experiments - against mouse SRF).

      However, after a more close investigation with individual siRNAs from these pools, I came to a conclusion that the observed necessity of both MRTF forms was caused by off-target effects of some of the individual siRNAs (at least in my system):

      a) Three of the MRTF-A siRNAs also reduced mRNA levels of MRTF-B. Only one was true anti-MRTF-A siRNA (and this one also gave the highest reduction of MRTF-A mRNA levels) but it didn't reduce the reporter induction in U2OS cells in marked contrast to the pool.

      b) One of the anti-MRTF-B siRNAs caused some general off-target effects in addtion to MRTF-B knockdown: considerable cell death, blocked not only SRF but also some other pathways. Its effect on SRF-luc persisted even when the target site in MRTF-B was mutated to prevent the targeted silencing. Three other siRNA prevented most of the SRF reporters's induction and it was reduced further by adding the good single anti-MRTF-A siRNA.

      The overall conclusion was that at least in U2OS cells the MRTF-A is not essential in these reporter settings but shows a minor partial contribution if MRTF-B is depleted.

      I'll probably include this data in the later paper but for now I hope these notes will be helpful for people using these MRTF/SRF SmartPools. I strongly recommend to check the effects of individual siRNAs in them.

      By the way, one of the siRNAs in human/mouse SRF pools also showed noticeable off-target cellular toxicity (and it was not even the strongest in reducing SRF mRNA levels). Given that each of the 3 pools I've worked with had some kind of off-target effect, this confirms the warnings of Jackson AL, 2010 that this can happen quite often. :( Thus, it seems that in general it is highly desirable to check all the individual siRNAs in commercial pools for target/off-target effect and have at least 2-3 different siRNAs against the same gene confirming the knockdown phenotype.


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    1. On 2014 Oct 18, David W Brandes, MS, MD, FAAN commented:

      I am very happy to see more published information about this topic. I have been speaking professionally abut this topic for 10 years and it is becoming increasingly recognized as to it's importance in the management of MS patients. This article confirms the often unrecognized frequency of this issue. When MS patients say they "are tired all the time," we need to think about the details. Physical fatigue, cognitive fatigue, psychological fatigue (depression) and sleepiness may all be part of this complaint.


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    1. On 2014 Oct 31, Francisco Felix commented:

      One of the major concerns about the data in this paper is the prior probability of the results reflecting the truth. Antineoplastons have no scientific basis better than homeopathy or psychic surgery. Hence, the prior probability associated with the results of this paper should be so small that a bayesian correction of its estimates (by the way, they were not even reported!) must invalidate its results. Try again (actually, don't!).


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    1. On 2017 May 01, Doug Berger commented:

      LACK OF BLINDING IN THIS STUDY WAS A SERIOUS METHODOLOGIC FLAW. ADDITIONALLY, FACULTY SUPERIOR OF LEAD AUTHOR STEVEN HOLLON, DR.STEPHAN HECKERS, EDITOR OF JAMA PSYCHIATRY, BOTH AT VANDERBILT DEPT. OF PSYCHIATRY REQUIRES REPORTING AS CONFLICT OF INTEREST

      This study by Hollon et al. compared an antidepressant medication-only arm with a combined cognitive therapy/antidepressant arm and concluded that the cognitive therapy/antidepressant combination enhanced the recovery rates compared with antidepressant alone, and that the magnitude of this increment nearly doubled for patients with more severe depression.

      We opine that for subjects with greater severity, there could have been both antidepressant efficacy, as well as more hope and expectation as bias in the group who knew openly that they had received combined cognitive therapy/medication as a possible treatment. This can lead to an erroneous conclusion of greater efficacy for the combined group. The large subject number in this study could also easily lead to an erroneous finding on statistical testing as a small amount of bias in the subjects adds-up.

      In addition, it goes against clinical trial logic to compare the unbilnded-cognitive therapy/medication group to the unblinded medication-only group.This is because, as all the study arms were unblinded, the combined cognitive therapy/medication group has an advantage over the medication-only group. The combined group does not filter any hope or expectation bias that may be lurking in the cognitive therapy arm, while the medication-only group engenders no different hope or expectation than the medication arm in the combined group. It is thus logically invalid to compare the cognitive therapy-medication arm that can have an unfiltered cognitive therapy-positive bias from the unblinded nature of receiving cognitive therapy tasks by cognitive therapy trained therapists vs. the medication-only arm which has the same bias possibility as the medication in the combined group, but lacking any possible positive bias from the combined cognitive therapy arm. Medications are required to show efficacy when compared in a double-blind study that includes a blind-placebo control as these controls are necessary to filter bias of any hope or expectation of efficacy. Neither blind controls nor blinded placebo were used in the design of the Hollon et al. study here.

      Dr. Hollon should have also noted the conflict of interest in that the Director of his dept. Dr. Stephan Heckers was also on the Editorial Board of JAMA Psychiatry when this paper was submitted and was the Editor-in-Chief of JAMA Psychiatry when it was published.

      The paper was retracted once for multiple errors, and it should be withdrawn completely because of poor clinical trial logic in making claims from unblinded subjects and treaters, and in addition due to conflict of interest in having the Editorial Director (Stephan Heckers) of the publication (JAMA Psychiatry) also as head of the Faculty of the lead author's (Hollon) affiliation at Vanderbilt University.

      The full comment on the Hollon et al. study above can be read here;

      Double blinding requirement for validity claims in cognitive-behavioral therapy intervention trials for major depressive disorder. Analysis of Hollon S, et al., Effect of cognitive therapy with antidepressant medications vs antidepressants alone on the rate of recovery in major depressive disorder: a randomized clinical trial. By D. Berger. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4863672/


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    2. On 2016 Apr 22, Ivan Oransky commented:

      This paper has been retracted and replaced: http://retractionwatch.com/2016/04/21/authors-retract-replace-highly-cited-jama-psych-paper-for-pervasive-errors/


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    1. On 2014 Aug 22, Hilda Bastian commented:

      It's great to see such a thorough and rigorous body of work on this subject. This group provides a good overview of the portion downsizing issue, and the limited evidence base on interventions, at Vermeer WM, 2014.

      A key part of the intervention in this trial (Poelman MP, 2015) is the interactive web-based PortionSize@warenessTool. Its development and trialing is described at Poelman MP, 2013, with these elements: background reading, an interactive flash game with photos of popular food products in the Netherlands, a flash game where you can upsize/downsize portions on screen, self-test score, information on portions for children and more.

      It would be helpful if details about the availability of this intervention could be provided (e.g. where it can be viewed, if the code is open source, and if the license allows translation). The TIDieR checklist (Hoffmann TC, 2014) - the template for intervention description and replication - is a good framework for this. More details on the components of interventions is important for enabling better practice (Glasziou P, 2010).


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    1. On 2014 Sep 23, Jorge Zorzopulos commented:

      Own to the importance of the Ebola outbreak dramatically described in this paper, scientists having any likely tool that could help should have a proper channel to offer it for humanitarian reasons. However, I found extremely difficult to find such proper channel. Could the authors clarify this situation. Thank you very much Dr. Jorge Zorzopulos Buenos Aires Argentina


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    1. On 2014 Aug 23, George McNamara commented:

      Terrific: renewable meat! Anolis looks pretty small, good for 'bite size renewables'. If Komodo dragons use the same pathways - or can be ZFN/TALEN/Cas9-sgRNA'd to do so, renewable Dragon meat!


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    1. On 2016 Jan 08, Anne Niknejad commented:

      "Two MAGL isoforms are reported in the GenBank (long isoform 1; 313 amino acids, accession code NP-001003794 and short isoform 2; 303 amino acids, accession code NP-009214) (Labar et al., 2010)."

      Error, correct references should be:

      NP_001003794 303 aa linear PRI 15-MAR-2015

      http://www.ncbi.nlm.nih.gov/nuccore/NM_001003794.2

      this sequence corresponds to the canonical UniProt sequence isoform 1 (http://www.uniprot.org/uniprot/Q99685)

      and

      NP_009214 313 aa linear PRI 15-MAR-2015

      http://www.ncbi.nlm.nih.gov/protein/6005786

      this sequence corresponds also to UniProt isoform 1 but with initial Methionine as in UniProt isoform 2, that means longer

      • METGPEDPSS

      (303 aa + 10 aa = 313 aa)


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    1. On 2015 May 17, Maya Guglin commented:

      Yes - adjusted for all classes of HF meds. Thanks for reading me so thoroughly! I think this is a really interesting topic.


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    2. On 2015 May 17, David Keller commented:

      Was the effect of CHF on type 2 DM adjusted for the use of thiazide diuretics, which promote insulin resistance?

      Thiazide diuretics are used widely by congestive heart failure (CHF) patients, either alone or in combination with loop diuretics (for synergy). Thiazides are well known to decrease insulin sensitivity and lead to impaired fasting glucose and frank type 2 diabetes. Was this medication side-effect adjusted for in the calculations showing that CHF increases the risk for type 2 diabetes ??


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    1. On 2014 Aug 27, Ryan Radecki commented:

      Post-publication commentary:

      Hypoxia & Overtreatment in Bronchiolitis

      “Treat the patient, not the number” works for many things in medicine – asymptomatic hypertension, hyperglycemia, and anemia, among others. However, hypoxia is less frequently dismissed as clinically irrelevant.

      And, that perfectly explains the results in this study, which evaluated clinician dependence on oxygen saturation to guide disposition in pediatric bronchiolitis....

      http://www.emlitofnote.com/2014/08/hypoxia-overtreatment-in-bronchiolitis.html


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    1. On date unavailable, commented:

      None


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    2. On 2014 Aug 26, Jorge H Ramírez commented:

      "Why hasn’t the intensity of scrutiny on financial interests been extended to non-financial interests ie, the ones that are far more prevalent and more strongly associated with publication misconduct?" -- Woolley K.

      Response:

      Financial conflicts of interests & their association with less retractions is not definitive evidence of more research misconducts by persons like me (i.e., non-financial conflict of interests).

      Two open questions:

      (1) How many requests of retractions for human research sponsored by pharmaceutical companies are not even openly discussed because libel laws? Re: I don't know. http://www.senseaboutscience.org/pages/keep-libel-laws-out-of-science.html

      (2) How many requests of retractions are not even eligible for open scientific debate? Re: I only know one which was requested & retracted by myself. However, question thread remains open.(1)

      Addendum to the original PubMed commons post: I just found an article describing similar cases to the situation described (yesterday) in the second question above. URL: http://www.bmj.com/content/341/bmj.c6985


      Jorge H. Ramírez. MD, MSc, PhD. Professor of Pharmacology Universidad del Valle http://chaoticpharmacology.wordpress.com/about/ Twitter: @jorgehernnramre

      References

      1. Ramirez, Jorge H (2014): Requested (Jul 29, 2014) & Retracted by the author (Aug 23, 2014): "Conelly S, et al. Dabigatran versus Warfarin in Patients with Atrial Fibrillation. N Engl J Med 2009; 361:1139-1151"] - Question Thread Open. figshare. http://dx.doi.org/10.6084/m9.figshare.1144305 Note: raw data is available in this fileset

      My conflict of interests related to this response are described in the following URLs: http://www.bmj.com/content/348/bmj.g1888/rr/763197 http://www.bmj.com/content/347/bmj.f4386/rr/763130 http://www.bmj.com/content/347/bmj.f1880/rr/763200


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    3. On 2014 Aug 25, Karen Woolley commented:

      .

      “No competing interests to declare”…oh really?

      The intensity of scrutiny of financial competing interests (eg, pharmaceutical industry sponsorship of research) is understandable – there have been enough high-profile cases of financial interests associated with publication misconduct to warrant concern. But…high-profile does not equate to high-frequency…indeed, the evidence (yes, evidence) on publications retracted for misconduct reveals that most retractions for misconduct occur for publications WITHOUT declared industry support (Woolley KL et al., Curr Med Res Opin 2011). A quick look at Retraction Watch supports the ongoing problem with non-financial interests and publication misconduct. The editors of PLoS Medicine highlighted the dangers of non-financial competing interests years ago:

      “Like all human activity, academic research and scientific publishing are inherently subjective, imperfect, and prone to bias, corruption, and self-interest. Indeed, because professional affinities and rivalries, nepotism, scientific or technological competition, religious beliefs, and political or ideological views are often the fuels for our passions and for our careers, private competing interests are perhaps even more potent than financial ones.” The PLoS Medicine Editors (2008) Making Sense of Non-Financial Competing Interests. PLoS Med 5(9): e199. doi:10.1371/journal.pmed.0050199

      When authors disclose “no competing interests to declare” what does that mean? Who is checking that nothing means nothing? Why hasn’t the intensity of scrutiny on financial interests been extended to non-financial interests ie, the ones that are far more prevalent and more strongly associated with publication misconduct?

      Our risk-management strategy for reducing the risks of interest-driven biases is rather risky. When will we prioritise strategies to manage the most prevalent and dangerous interests – the non-financial ones?

      Professor Karen Woolley PhD Certified Medical Publication Professional (Twitter: @kwproscribe)

      Disclosures

      Non-financial: Advocate for ethical publication practices, regardless of sponsor (for-profit, not-for-profit), Director of the International Society for Medical Publication Professionals and Chair of its Asia-Pacific Advisory Committee; active member of other not-for-profit organisations providing education on ethical publication practices. Author of peer-reviewed publications on ethical publication practices.

      Financial: Employee of ProScribe - part of the Envision Pharma Group (providing ethical publication planning and medical writing services to authors and sponsors worldwide - we do NOT ghostwrite)


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    1. On 2014 Sep 02, Hilda Bastian commented:

      An excellent overview of the need for studying humor in science communication, and the academic challenges in it. While there’s some more evidence than that gathered here, I think Hauke Riesch’s conclusions about the uncertainties of benefit and harm are spot on.

      I found the review on studies of humor in teaching he points to (Banas, 2011) helpful as well. From children through to continuing education and the communication of science among peers (Rockwood K, 2004), there’s a lot to learn here.

      In describing the varying results of studies, Riesch doesn’t explicitly address a key confounder in communication research: the quality of the intervention. It’s hard to make sense of bodies of evidence in this field without quality assessments and being able to see the interventions (Glasziou P, 2010). Skill in using humor may account for some of the heterogeneity. And learning about the skills necessary for effectiveness – and how to acquire them – are key issues in this field, too.

      Riesch addresses well the potentially alienating and stereotyping effect of science humor, as well as the potential benefits of social group cohesion. In addition, though, satire in peer-to-peer communication and for policy-related issues is also a critical element of humor in science communication, as it is in other areas of community life (Zyglis, 2003).

      I welcome the author’s desire to “open a discussion” on humor in science communication. But this article being behind a paywall isn’t going to help that process. It would be great to know if the author is engaging with discussion in any other forum.

      I’ve blogged about the science of humor, and humor in science, in response to this article at Scientific American.


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    1. On 2015 Jul 12, Weijun Liu commented:

      There is a comment on this paper in Pubpeer, possible duplicated data published in their later Cripsr/cas9 E6 paper.


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    1. On 2016 Nov 25, Darya Vanichkina commented:

      I was trying to reproduce the results of this study, but was unable to do so.

      The information for overall survival, TCGA subtype and treatment status is not available in the Supplementary tables, or as part of the Chinese Glioma Genome Atlas.

      Would it be possible for the authors to provide this information, perhaps in GEO or via the Chinese Glioma Genome Atlas web portal?


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    1. On 2014 Dec 03, Rafael Najmanovich commented:

      We predicted back in 2012 (Chartier M, 2012) as part of a large scale analysis of rare codon cluster that such clusters may play a role in the molecular recognition of the nascent protein for intracellular targeting and membrane insertion. It is unfortunate that the authors were not aware of our publication.


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    1. On 2014 Sep 04, Kenneth Witwer commented:

      This review covers an important area of research, as saliva is obtained non-invasively and extracellular vesicles including exosomes may be enriched in useful biomarkers. Unfortunately, several apparent errors are repeated throughout the review.

      -The type of extracellular vesicle known as an "exosome" is not the same entity as the nucleic acid processing complex of the same name. A confusion of the two seems evident here. Readers will need to consult the sources to determine what information is and is not relevant to extracellular vesicles.

      -Intra- and intercellular vesicle trafficking are also conflated, with the Suedhof/Schekman/Rothman Nobel Prize research described as focused on exosomes. Secretory and secreted vesicles are certainly related, but they are distinct.


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    1. On 2015 Feb 27, Geriatric Medicine Journal Club commented:

      This study looks at atypical antipsychotics and the risk for acute kidney injury in older adults. This paper was critically appraised at the September 2014 Geriatric Medicine Journal Club (follow #GeriMedJC on Twitter). A full transcript of the discussion can be found at http://gerimedjc.blogspot.com/2014/09/to-two-articles-critically-appraised.html?spref=tw Our colleagues from the Nephrology Journal Club (follow #NephJC on Twitter) also chimed in. In general, growing concern regarding the use of atypical antipsychotics.


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    1. On 2014 Sep 01, Ferenc Zsila commented:

      The authors claim that in relation to physiological conditions, cancer cells have substantially lower, acidic intracellular pH.

      Abstract: "...under acidic conditions (pH 5.0) mimicking the intracellular pH-conditions."

      In page 364: "Specifically, the intracellular pH of tumor cells (pH 5.0-6.5) is usually much lower than physiological pH conditions (pH 7.4), which has encour-aged researchers to develop pH-responsive prodrug formulations to improve therapeutic efficacy."

      In contrast to this statement, numerous data show that just the opposite is true: the intracellular pH of cancer cells is modestly alkaline (pH~7.4). Not the intra- but the extracellular milieu of tumours is acidic. Intracellular acidosis leads to cell death.

      Reference: Webb BA, 2011


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    1. On 2014 Sep 01, Amanda Capes-Davis commented:

      The authors describe KB as an epidermoid cell line. Although this term is widely used, it is not accurate for this cell line. KB is known to be cross-contaminated with HeLa and thus is a cervical adenocarcinoma cell line. It is not an oral squamous cell carcinoma (epidermoid carcinoma) as was originally thought.

      KB is a widely used model for multidrug resistance. To help scientists who might use KB for other applications, it would be helpful if authors can refer to KB as a HeLa derivative, and to avoid the terms epidermoid, squamous cell carcinoma, or oral.

      I note that the authors performed authentication testing. The information above would help readers to make sense of their test results. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2016 Apr 22, Kenneth Witwer commented:

      My co-authors and I found no uptake of milk miRNAs, examining the same samples reported in this paper as well as public sequencing data from these samples, Shu J, 2015. The findings encompass the two miRNAs reported by Baier et al, which are homologous in human and cow and could not be assigned to source or human by the methods of the paper, and a variety of additional miRNAs, even uniquely bovine miRNAs. It appears that both previously offered hypotheses for the observations of Baier, et al are now unsupported: the exogenous uptake hypothesis and my hypothesis, glucose-mediated regulation of endogenous RNA, Witwer KW, 2014. Instead, as also supported by rigorous experiments with genetically manipulated mouse models, Laubier J, 2015, Title AC, 2015, milk miRNAs, like other dietary RNAs Witwer KW, 2014, Dickinson B, 2013, Snow JW, 2013, do not appear to reach biologically meaningful levels in circulation, whatever this might mean, or indeed be taken up at all through the intact mammalian gut.


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    1. On 2014 Sep 15, Amanda Capes-Davis commented:

      The authors use the cell line HEp-2 to look at sensitivity to cisplatin. Please be aware that HEp-2 is cross-contaminated with HeLa, a cervical adenocarcinoma cell line. Results obtained from HEp-2 do not relate to laryngeal carcinoma.

      Cell lines can be tested for cross-contamination through consensus methods such as short tandem repeat (STR) profiling. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2014 Nov 11, Serge Ahmed commented:

      This comment is a follow-up of my previous comment about the difficulty in interpreting this study that contradicts most previous similar studies. After a careful analysis of this paper and after collecting all elements of methods “ectopically scattered” through the text, I think I finally arrived at a satisfactory explanation for why most rats preferred cocaine over sweet water in the present study. Briefly, everything was made to make access to sweet water reinforcement less direct and more difficult than access to cocaine reinforcement, thereby biasing choice towards cocaine!

      More specifically, rats had to go through an unusually long chain of behavioral events before getting access to sweet water. A similar chain was not required for cocaine delivery. First, once rats turned the wheel on the operant panel, they had to cross the cage to reach a magazine on the opposite panel inside which there was a retractable drinking spout that delivered sweet water. This arrangement introduces a spatial and thus a time gap between responding and sweet water reinforcement. Both gaps are known to reduce conditioning. Second, once rats have reached the magazine, they did not have directly access to the drinking spout that delivered sweet water. They had first to insert their head into the magazine to make the retractable drinking spout appears. This behavior amounts to a second operant response which thus defines with the first response (i.e., wheel turning) an operant chain. In addition, once rats inserted and maintained their head in the magazine, the drinking spout was not continuously available but came “back and forth in the magazine during 50s.” This is a rather unusual method of fluid delivery (note: the frequency and duration of these back-and-forth movements are not indicated in the Methods).

      Thus, to repeat, everything was made in the present paper to make access to sweet water reinforcement more difficult and less direct than access to cocaine reinforcement, thereby biasing choice towards cocaine. This unusual approach may be appropriate for addressing some scientific questions but it is misguided and inappropriate for studying the vulnerability to cocaine addiction which was the main goal of the present paper. If one wants to pursue such a goal, one better tries to make access to cocaine reinforcement equal to or more difficult than access to the nondrug option and not the other way around! Indeed, if one sufficiently weakens the nondrug option, then one will eventually reach a point where most individual rats, even the non-addicted ones, will prefer the drug! To take an extreme example, if one provides rats with ready access to cocaine but ask them to play piano or climb Mt Everest to get access to sweet water, they will surely choose cocaine over sweet water. This is not surprising, this is just trivial! In contrast, if rats take cocaine despite and at the expense of an equally or a more accessible potent nondrug option, then one has got something much less trivial and probably more relevant for studying the vulnerability to cocaine addiction.


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    2. On 2014 Aug 22, Serge Ahmed commented:

      This study is interesting and also quite embarrassing. It is interesting because of the important questions that it asks. It is embarrassing because it shows that when given a choice, most rats prefer cocaine over sweet water – a finding that is strictly the opposite of what we and others have found over the past few years. Of course, contradiction and refutation are the “game of science”. We should not be embarrassed by them and instead welcome them.

      My embarrassment comes from the fact that these opposite outcomes were obtained by a former master student of mine – Nathalie Vanhille who is the first author of this study – using a choice protocol initially developed in our lab. When Nathalie was working in our lab using this protocol, she observed that most rats preferred sweet water over cocaine – the opposite of what she now reports in this study despite the use of an identical choice protocol.

      But were the choice protocols really identical? Of course not! Like always, the devil lurks into the details and details can sometimes matter a lot! Apparently, this study differs from our previous choice studies in the way rats were given access to sweet water. In our study, access to sweet water was pretty straightforward. Rats had to press a lever to fill a nearby receptacle with sweet water. Then they could obtain additional volumes of sweet water during 20s by continually licking the receptacle. In this study, however, access to sweet water was really contrived for reasons that remain unclear until one reaches the middle of the Discussion. In fact, despite my best efforts and those of other members of the team, we were unable to get a clear final picture of how rats get access to sweet water in this study.

      So here is my challenge for the interested readers and researchers: I would really appreciate if someone could help me figure out how exactly rats get access to sweet water in this study.

      Thank you!


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    1. On 2014 Sep 10, Suleyman Serdar Koca commented:

      I thank the comment first of all. The evaluation of serum IL-33 levels was not the primary aim of the present study. It was analyzed in limited patients to determine whether IL-33 gene polymorphisms affect serum IL-33 level. However, the detected relations of serum IL-33 level with the clinical signs were reported. Behçet’s disease has complex ethiopathogenesis. Genetic basis of the disease is divergent. Not only patients with different ethnic origins but also each patient has different disease burden. Therefore, the results of cytokines may be divergent in the different cohort.


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    2. On 2014 Aug 26, Kamel Hamzaoui commented:

      Recently an interesting paper was published in Brain Behv Immunology about IL-33 in the CNS


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    3. On 2014 Aug 26, Kamel Hamzaoui commented:

      Interesting paper. I cannot understand how the authors found similar IL-33 levels in BD patients than in healthy controls (52 patients were studied). They also found increased levels of IL-33 in BD patients with uveitid (32 patients were studied). We found the same increase of IL-33 in BD patients with retinal uveitis. We and others found increased levels of IL-33 in serun, in cerebrospinal fluid and in EN skin lesions measured at the mRNA and immunohistology.

      Our laboratory and the Korean laboratory used the same Kit Elisa, but not the authors. The authors of the paper have to study control disease such as RA, SLE, MS patients.

      Thank you


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    1. On 2017 Nov 12, Gerardo Ferbeyre commented:

      I have red this paper many times and I find always inspiration for experiments and new ideas. The authors condensed a tremendous body of work while keeping their main message beautiful and simple. In pancreatic cancer, inhibition of the RAS/MAPK pathway allows the emergence of a subpopulation of dormant tumor stem cell with increased dependency on mitochondria. We have reproduced many of the key characteristics of these pancreatic cancer stem cells using a different experimental model and I wonder whether this phenotype is unique to these cancer cells when they evolve or whether the cells are reactivating a primitive embryonic program of pancreatic epithelial stem cells.


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    1. On 2014 Nov 24, Guillaume Filion commented:

      This article is one of the "CISCOM meta-analyses", which are very similar papers written by different authors. For more information about the CISCOM meta-analyses, check the blog post "A flurry of copycast on PubMed" at the following link http://blog.thegrandlocus.com/2014/10/a-flurry-of-copycats-on-pubmed


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    1. On 2014 Aug 27, Ryan Radecki commented:

      Post-publication commentary:

      "Should the 48-hour Cardioversion Window Be Revised?"

      It has become generally accepted practice to treat new-onset atrial fibrillation and atrial flutter with electrical cardioversion in the acute setting – provided the known onset of atrial fibrillation is less than 48 hours. Beyond that, caution tends to be advised – whether through use of transesophageal echocardiography to rule out left atrial thrombus, or through pre- and post-procedural anticoagulation.

      However, this data from a research letter in JAMA suggests – possibly we ought to be even more cautious regarding time-of-onset....

      http://www.emlitofnote.com/2014/08/should-48-hour-cardioversion-window-be.html


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    1. On 2014 Sep 15, Gaetano Santulli commented:

      In this elegant retrospective cohort study Gialdini and colleagues report that among patients hospitalized for surgery, perioperative atrial fibrillation is associated with an increased long-term risk of ischemic stroke, especially following noncardiac surgery. To predict cumulative rates of ischemic stroke the Authors used the CHA2DS2VASc score. Remarkably, in the low-risk categories (score≤1) there are 13 and 9 strokes among patients undergoing cardiac and noncardiac surgery, respectively. The Authors however do not provide any information about baseline electro-, echocardiographic or cerebrovascular assessment for these subjects. Thus, clinical data on potential cardiac (inter-atrial septum defect, mitral valve stenosis, cardiomyopathies) and cerebrovascular alterations, in our opinion essential for interpreting the results provided, are missing. This aspect is particularly relevant since the above-mentioned disorders are functionally related to ischemic stroke (1,2) and might exert pro-thrombotic effects also in low-risk subjects. Moreover, diabetes mellitus has been shown to be an independent risk factor for stroke, including in patients with low CHA2DS2VASc score (3). In this sense, it would be interesting to know the percentage of diabetic patients in the low-risk population. Equally important, a more comprehensive assessment of the baseline coagulation status could be useful: given the lack of data on antithrombotic therapy, acknowledged by the authors in the limitations of the study, it would be helpful to the Reader to know at least the rate of hemorrhagic stroke events.

      References 1. McCabe DJ, Rakhit RD. Antithrombotic and interventional treatment options in cardioembolic transient ischaemic attack and ischaemic stroke. J Neurol Neurosurg Psychiatry. 2007 Jan;78(1):14-24. 2. Finsterer J, Stollberger C. Stroke in myopathies. Cerebrovasc Dis. 2010;29(1):6-13. 3.Marfella R, Sasso FC, Siniscalchi M, Cirillo M, Paolisso P, Sardu C, Barbieri M, Rizzo MR, Mauro C, Paolisso G. Brief episodes of silent atrial fibrillation predict clinical vascular brain disease in type 2 diabetic patients. JACC. 2013;62(6):525-30.

      Celestino Sardu, MD (1), Gaetano Santulli, MD, PhD (2) (1) Second University of Naples, Naples, Italy; (2) Columbia University Medical Center, New York, NY, USA

      Conflict of interest: none.


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    1. On 2015 Jan 01, Prashant Sharma, MD, DM commented:

      Please note that these extremely precious specimens in these tiny humans were obtained by trained pathologists, and not neonatologists, pediatricians or radiologists.

      Just as is the case for fine needle aspirates, the best bone marrow specimens with highest diagnostic yields and lowest inadequacy rates come when pathologists themselves take the specimen they are to subsequently analyze.

      There are of course many other issues (logistic, training, regulatory, safety) that are tied up with this fact, but the above, in my experience, is invariable.


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    1. On 2014 Oct 27, Maria Flavia Di Renzo commented:

      As mentioned in the paper and shown in Supplementary Figure 2, we also used different single shRNAs. Actually, we also used five shRNAs specific for different sequences of CDT2 and different from the sequences of the four siRNAs of the pool. We obtained regulation of CDT2 targets and commitment towards cell death in cancer cells but not in normal cells. However, the in-depth analysis of molecular targets and cell cycle was not feasible in cells stably committed to death. Thus we carried out experiments with siRNAs that resulted in similar, but transitory, biochemical and functional effects. In conclusion, we are confident that the observed phenotypes might be attributed to CDT2 suppression.


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    2. On 2014 Oct 17, Eugen Buehler commented:

      The authors cite our paper (Buehler E, 2012) as evidence that “…pools of siRNA targeting different mRNAs, such as those used in libraries, results in increased off-target effects”. Unfortunately, that sentence is not supported by our paper. The method demonstrated in our paper was applied to an arrayed screen of individual siRNAs in which there were no pools, and no conclusions about pooling of siRNAs can be reached from that manuscript. Furthermore, the authors state that “The use of this siRNA pool allows avoiding too high concentration of each single siRNA and thus prevents off-target effects” and cite Jackson AL, 2010 to support this. Again, this assertion is not supported by the cited reference. Jackson AL, 2010 states that “Pooling of multiple siRNAs to the same target may help to reduce off-target silencing, due to competition among the siRNAs in the pool” (emphasis added). No evidence exists to support the claim that pools 3 or 4 siRNAs will prevent off-target effects. To the contrary, we have demonstrated previously that pooling siRNAs does not generate more reproducible phenotypes than single siRNAs (see Marine S, 2012, Figure 1, B and C) and that pools of siRNAs can and do generate many off-target phenotypes, which can then be confirmed by deconvolution of those pools (see Marine S, 2012, Figure 2). Unfortunately, the authors base most of their conclusions on experiments using a single reagent (a pool of four different siRNAs targeting CDT2) and a single non-silencing control. This means that many or all of the phenotypes they observed experimentally may be due to siRNA off-target effects (see Chung HY, 2014 for a case study in how off-target effects can result in false positives). This is not to say that their conclusions are incorrect, only that I believe that RNAi experiments require multiple independently tested reagents and/or matched controls to guard against the false positives due to off-target effects that are so frequent in these experiments.


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    1. On 2014 Aug 28, Frederick K Korley commented:

      Agreed. Troponin values can no longer be used in a dichotomous fashion. Any troponin elevation is a bad troponin elevation. However, those without acute elevations may not necessarily need inpatient hospitalization. If they are discharged, they will benefit from expedited outpatient follow-up.


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    2. On 2014 Aug 27, Ryan Radecki commented:

      Post-publication commentary:

      "Highly Sensitive Troponins – False Positive Bonanza"

      The “highly sensitive” troponin has received a great deal of publicity, hyped ad nauseum, see: “Simple test could help rule out heart attacks in the ER.”

      But, as sensitivity increases – invariably, specificity decreases. However, that is not the fault of the test – it is a failure of clinicians to ask the correct question of the test. When asking “does this patient have an acute myocardial infarction?”(most commonly Type 1 MI in the ED), our training and education has been outpaced by assay technology – the test no longer provides a dichotomous “yes” or “no”.

      http://www.emlitofnote.com/2014/08/highly-sensitive-troponins-false.html


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    1. On 2014 Nov 02, Swapnil Hiremath commented:

      This systematic review, along with its accompanying review was discussed on Oct 21st 2014 in the open online nephrology journal club, #NephJC, on twitter. Introductory comments are available at the NephJC website. It was a great discussion, with more than 20 participants, including nephrologists, cardiologists and residents/fellows from different specialties. A transcript and a curated (i.e. Storified) version of the tweetchat are available from the NephJC website. The highlights of the tweetchat were:

      • The investigators and the funding agency (AHRQ) should be commended for attempting to answer these important questions about the role of troponins in patients with chronic kidney disease.

      • Most participants rely on a rise in troponin levels to help diagnose acute coronary syndrome in CKD patients, and were disappointed that no evidence was found to support (or refute) this practice.

      • The adverse prognostic implications of higher troponin levels, especially in asymptomatic CKD patients was thought to be quite concerning and was the subject of much discussion, with many possible therapeutic management options being raised.

      Overall, these reviews answered a few questions, but also brought out many areas where further research needs to be focused. Interested individuals can track and join in the conversation by following @NephJC or #NephJC, or visit the webpage at NephJC.com.


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    1. On 2014 Nov 02, Swapnil Hiremath commented:

      This systematic review, along with its accompanying review was discussed on Oct 21st 2014 in the open online nephrology journal club, #NephJC, on twitter. Introductory comments are available at the NephJC website. It was a great discussion, with more than 20 participants, including nephrologists, cardiologists and residents/fellows from different specialties. A transcript and a curated (i.e. Storified) version of the tweetchat are available from the NephJC website. The highlights of the tweetchat were:

      • The investigators and the funding agency (AHRQ) should be commended for attempting to answer these important questions about the role of troponins in patients with chronic kidney disease.

      • Most participants rely on a rise in troponin levels to help diagnose acute coronary syndrome in CKD patients, and were disappointed that no evidence was found to support (or refute) this practice.

      • The adverse prognostic implications of higher troponin levels, especially in asymptomatic CKD patients was thought to be quite concerning and was the subject of much discussion, with many possible therapeutic management options being raised.

      Overall, these reviews answered a few questions, but also brought out many areas where further research needs to be focused. Interested individuals can track and join in the conversation by following @NephJC or #NephJC, or visit the webpage at NephJC.com.


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    1. On 2014 Aug 12, Ryan Radecki commented:

      Post-publication commentary:

      "Just Another Advertisement for tPA"

      As with last week's coverage of the updated Cochrane Systematic Review for tPA in acute ischemic stroke, the key question is: what’s new?

      The first pooled meta-analysis, published in The Lancet in 2004, included NINDS, ECASS I, ECASS II, and ATLANTIS. It was subsequently updated in 2010 to add ECASS III and EPITHET. Now, these authors have decided to add IST-3.

      I am actually a huge fan of individual-patient meta-analyses. Depending on the data availability, the similarity of trial protocols, and other issues associated with heterogeneity, this is the gold-standard for aggregating data and increasing power. Individual-patient analyses also allow for more reliable exploration of subgroup effects not otherwise possible through regular meta-analyses or systematic reviews.

      But, at the crux of it, a meta-analysis is only as good as the included trials – and this is a topic much debated over the last twenty years....

      http://www.emlitofnote.com/2014/08/just-another-advertisement-for-tpa.html


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    1. On 2014 Aug 12, Jens Staal commented:

      Interestingly SNP rs147414021 corresponds to a R149Q mutation. It will be interesting to see whether this SNP is associated to disease.

      http://www.ncbi.nlm.nih.gov/projects/SNP/snp_ref.cgi?geneId=10892


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    1. On 2014 Nov 24, Guillaume Filion commented:

      This article is one of the "CISCOM meta-analyses", which are very similar papers written by different authors. For more information about the CISCOM meta-analyses, check the blog post "A flurry of copycast on PubMed" at the following link http://blog.thegrandlocus.com/2014/10/a-flurry-of-copycats-on-pubmed


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    1. On 2014 Nov 05, Fillip Port commented:

      This paper reports on the use of the H1 promoter to drive expression of gRNAs for CRISPR/Cas genome engineering. The authors demonstrate that gRNAs expressed from H1 can efficiently modify the genome of cultured human cells in conjunction with Cas9 endonuclease. Interestingly, gRNA expression levels from H1 are lower than from the commonly used U6 promoter. Although this can negatively effect mutagenesis rates at the on-target site, it can also increase CRISPR/Cas specificity, as high activity is more likely to lead to off-target effects. This makes the H1 promoter a potentially useful tool for CRISPR/Cas genome engineering in human cells.

      However, the authors suggest that their results have much more general significance by expanding the CRISPR/Cas genome targeting space. This is because the U6 promoter initates transcription at a G nucleotide (although see comment below and reference therein), which according to the authors constrains genomic target sites to GN19NGG. This assertion is surprising as it is common practice in the CRISPR field to target sites that do not start with a G by simply adding a (often mismatched) G to the corresponding gRNA or to replace the first nucleotide with a G to create a gRNA that is mismatched at the first position. The authors acknowledge these strategies in the first paragraph of their discussion, but cite six papers as providing evidence that 5’ extensions or truncations reduce gRNA efficiency. However, these papers in fact provide evidence that 5’ extensions or truncations of a single nucleotide often have no effect on activity and when they do the effect is usually minor (modified gRNAs usually retain >80% activity). Furthermore, the authors do not cite another study that shows that small gRNA truncations retain high activity in the majority of cases and have reduced off-target effects (Fu Y, 2014). Therefore, much of the published evidence suggests that extending or truncating gRNAs by a single nucleotide is well tolerated by the great majority of gRNAs. As a result it is in principle possible to target any genomic site adjacent to a PAM motif with gRNAs expressed from a U6 promoter and hence the H1 promoter, although potentially useful, does not expand the CRISPR target space.


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    2. On 2014 Aug 12, Haoquan Wu commented:

      The preferred initiation nucleotide for U6 promoter are A and G, as we have shown in our study which can be found http://www.nature.com/mtna/journal/v3/n5/full/mtna201412a.html. We also confirmed that gRNAs starting with A can disrupt the target gene at similar level as gRNAs starting with G in the study. H1 promoter is much weaker than U6, which might significantly lower the CRISPR-Cas9 system efficiency.

      It is amazing that the commonly accepted conceptions about U6 promoter initiation and termination are not complete although U6 promoter has been the most commonly used promoters to drive small RNA expression. The commonly accepted conception that the continuous Ts is the termination signal for U6 promoter is also not correct.


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    1. On 2015 Sep 10, Lydia Maniatis commented:

      The authors say that “we assessed whether the highest luminance is mapped onto a fixed surface reflectance (“white”) independently of target reflectance, illumination level (real or simulated), or luminance. ”

      Evidently, by “illumination level” they are referring to the collection of luminances of their “Mondrians,” and by “luminance” they are referring to the luminance of individual target surfaces. It may be that, in relatively low luminance conditions, observers experienced a sense of low illumination, but neither the authors nor anyone else has, to my knowledge, tested whether such an impression does, in fact, arise. The fact that “low illumination” conditions resulted in lower lightness matches for targets actually implies the opposite, since impressions that surfaces are “in shadow” typically cause them to appear lighter than equiluminant. apparently plain view surfaces. So average luminance (regardless of how the investigators achieve this) and contrast are the variables being looked at,

      As is typical in experiments using “Mondrians” or checkerboard stimuli, the authors seem to overlook the fact that these stimuli are capable of producing differential illumination, transparency, luminosity effects, despite the absence of the usual “cues.” This is evident, for example, in checkerboard stimuli used by Allred, Radonjic, Gilchrist & Brainard (2012), who tentatively acknowledge (but do not test for) some but not all of the (self-evident) effects. Anderson et al cite Radonjic, Allred, Gilchrist and Brianard (2011) as having shown that “a stimulus ratio of 5905:1 could be mapped onto an extended lightness ratio of 100:1 and concluded that such results ruled out theories that predict perceived lightness from luminance ratios or Weber contrast” and suggest that “these data cast significant doubt on the view that the visual system has any understanding of the range of reflectance values that populate natural environments.” However, it is not clear that the high-range stimuli in Radonjic et al's experiments did not produce luminosity effects. Their observers did, in fact, report luminosity for the highest luminance values in those stimuli, but the authors discounted those reports as being due to the stimuli having been presented on an “emissive screen.” However, this explanation does not seem credible given that the same luminance values did not produce luminosity reports in lower-range situations.

      If there were apparent scission effects going on in Anderson et al's stimuli, then observer reports would have been affected. When a surface is completed “beneath” a shadow, and seen as homogeneous in its lightness, this does not mean that we can't see that it is also darker at the shadowed place, in the same way that amodally completed surfaces are seen and not seen at the same time. You can't disprove that an amodal completion is occurring simply on the basis of asking an observer to report on the local color in the image at an “obstructed” location. Similarly, simply asking a naive observer to make a lightness match where scission is occurring is problematic.

      It is always important for readers of perception papers to be able to see the stimuli used, so it would have been good if all of the Mondrians, and not just the one, were made available.


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    1. On 2016 Sep 18, Daniel Schwartz commented:

      The ROKS nomogram can be used to predict recurrence of a second kidney stone via an online calculator or via a mobile app https://www.qxmd.com/calculate/calculator_3/roks-recurrence-of-kidney-stone-2014

      Conflict of interest: Medical Director, QxMD


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    1. On 2014 Aug 13, Amanda Capes-Davis commented:

      Unfortunately many cell lines are misidentified and do not correspond to the tissue from which they were thought to be established. This is the case here: both HEp-2 and KB are cross-contaminated by HeLa, a cervical adenocarcinoma cell line. For a list of known cross-contaminated or otherwise misidentified cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2015 Mar 28, Amit Kumar Chowhan commented:

      Dear Sir,

      We read the article by Srikanth S et al.<sup>1</sup> on ‘A comparative study of fine-needle aspiration cytology (FNAC) and fine-needle non-aspiration cytology (FNNAC) techniques in head and neck swellings’ with interest and appreciate the inclusion of multiple organs i.e. lymph node, thyroid and salivary gland located in head and neck region in the study. Although fine needle aspiration cytology is a well-established tool as a first line diagnostic modality, however, a major criticism pertains to its use in highly vascular organs such as thyroid and liver, or in haemorrhagic lesions where large quantities of blood compromise cytologic interpretation. Hence we agree with the authors when they excluded lesions of vascular origin from their study.

      We agree with the authors that FNNAC allows greater ease of sampling with better control of the hand during the procedure and a good perception of the lesion consistency, enabling more precise entry into the mass and thus is more user friendly. Apart from being less traumatic and painful to the patient, as suggested by the authors, we would like to add that with this technique the patient would also be less apprehensive about the procedure, when a large syringe with needle and a syringe holder is not seen, thus making FNNAC more patient friendly. Another advantage of FNNAC is that the syringe is used to expel the material after the procedure is completed, whereas in FNA it is used to create a suction force to aspirate the cells in to the needle. A fresh sterile syringe is therefore not necessary for FNNAC, thus reducing the cost of procedure.

      In their study the authors concluded that for thyroid lesions the non-aspiration technique was better than aspiration technique with respect to all the five parameters proposed by Mair et al.<sup>2</sup> i.e. background blood/clot, amount of cellular material, degree of cellular degeneration & trauma and retention of appropriate cellular architecture. In a similar study conducted by us<sup>3</sup> on thyroid lesions, we found that the non-aspiration technique was better in relation to all the parameters except for amount of cellular material, which was better with aspiration technique. In cases of colloid goiter, brownish colloidal fluid drained out immediately on putting needle and drenched the fingers holding the needle. This problem was handled by keeping a syringe ready, which was immediately attached to the needle and the fluid collected in the syringe – to be cyto-centrifuged for better cellularity. Another problem encountered was for calcified nodules, which required vigorous aspiration, as it didn’t yield any material on non-aspiration. We therefore, would recommend first non-aspiration technique to be performed and if the material obtained is insufficient then only to go for another pass with aspiration technique.

      References:

      1.Srikanth S, Anandam G, Kashif MM. A comparative study of fine-needle aspiration and fine-needle non aspiration techniques in head and neck swellings. Indian J Cancer 2014;51:98-9.

      2.Mair S, Dunbar F, Becker PJ, Du Plessis W. Fine needle cytology - is aspiration suction necessary? A study of 100 masses in various sites. Acta Cytol. 1989;33:809-13.

      3.Chowhan AK, Babu KV, Sachan A, Rukmangdha N, Patnayak R, Radhika K, Phaneendra BV, Reddy MK. Should we apply suction during fine needle cytology of thyroid lesions? A prospective study of 200 cases. Journal of Clinical and Diagnostic Research 2014;8:19-22.


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    1. On 2014 Sep 01, Amanda Capes-Davis commented:

      The KB cell line is often used to test therapeutic activity against cancer. But although KB comes from cancer, it is not oral squamous cell carcinoma. KB is known to be cross-contaminated with HeLa and is actually cervical adenocarcinoma. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2014 Sep 01, Graham Coop commented:

      Here is a post on some of the difficulties of interpreting positive signals of polygenic selection found by our approach: http://gcbias.org/2014/08/07/some-thoughts-on-our-polygenic-selection-paper/


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    1. On 2014 Aug 18, David Keller commented:

      Ibuprofen, but not other NSAID's, is associated with decreased risk of Parkinson's disease

      Ibuprofen use has also been observed to be strongly associated with a lower risk of incident Parkinson's disease (1). Other NSAID's, such as naproxen, have not showed any such apparent protective effect (2). Given that long-term use of NSAID's "such as ibuprofen" has been observed to be associated with "reduced risk and delayed onset of Alzheimer's disease", I would be cautious about substituting a different NSAID, such as flurbiprofen, unless it has also demonstrated the same associations with reduced Alzheimer's risk, because the epidemiological studies of NSAID use and Parkinson's risk have indicated that, when it comes to the risk of neurological degeneration, different NSAID's can have vastly different effects.

      References

      1: Gao X, Chen H, Schwarzschild MA, Ascherio A. Use of ibuprofen and risk of Parkinson disease. Neurology. 2011 Mar 8;76(10):863-9. doi: 10.1212/WNL.0b013e31820f2d79. Epub 2011 Mar 2. PubMed PMID: 21368281; PubMed Central PMCID: PMC3059148.

      2: Driver JA, Logroscino G, Lu L, Gaziano JM, Kurth T. Use of non-steroidal anti-inflammatory drugs and risk of Parkinson's disease: nested case-control study. BMJ. 2011 Jan 20;342:d198. doi: 10.1136/bmj.d198. PubMed PMID: 21252104; PubMed Central PMCID: PMC3023971.


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    1. On 2014 Aug 19, Sameer Agnihotri commented:

      Dear Dr. Li, the uncorrected proof is currently online. Figure 7 will be corrected soon for the final edited version. Thank you for your observation.


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    2. On 2014 Aug 12, Mengxia Li commented:

      In Figure 7, the authors listed LIG4 as BER gene by mistake which is not a typical BER gene and functioning in NHEJ.


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    1. On 2014 Nov 27, Mangesh Thorat commented:

      Our systematic review of harms associated with aspirin use is now published (Thorat MA, 2015). Also recently published is our detailed response (Thorat MA, 2015) to Elwood P, 2015, who suggest that we have overestimated aspirin’s harms.


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    2. On 2014 Aug 22, Mangesh Thorat commented:

      Response to Hilda Bastian’s recent comment:

      Thank you for the continued discussion. Individual studies like PHS did report a 5-year follow-up, which is not uncommon. Rothwell’s recent overview (Rothwell PM, 2012) did look at studies with shorter follow-up, but the central question in this overview was aspirin’s effect on incidence. The effect on incidence starts to appear at 3 years, while that on mortality takes about 5 years. On the other hand, for example, the endpoint Seshasai SR, 2012 used was mortality and not incidence and therefore they could not observe a significant reduction. Sutcliffe P, 2013 looked at all these data and treated them as equal. Additionally, they did not have access to updated WHS results that showed a significant reduction in CRC. This resulted in their excessive perception of uncertainty; it is prominently reflected in their interpretation.

      We believe that most experts agree that "the evidence supporting aspirin's benefits on cancer is now overwhelming.", the differences in opinion probably only exist for the magnitude and site-specific effects (e.g. 3 of our co-authors). This is the reason we provide several sensitivity analyses that use lower magnitude of benefits, higher magnitude of harms and also lack of effect on certain cancer sites. All these show a net benefit.

      We agree that long-term harms should not be easily dismissed, but we believe that the severity of harms also needs to be considered in any assessment. In our assessments, we have erred on the side of caution and very likely over-estimated the harms. Individual circumstances differ, and therefore we believe that a careful assessment by and an informed discussion with a healthcare professional is necessary.

      We also look forward to the new USPSTF review as we have been informed that on this occasion USPSTF will look at the overall picture by assessing impact on all diseases/conditions affected by aspirin and not just single disease/disease group.

      Response to David Colquhoun’s comment:

      Please note that the NHS Choices comment has been amended to delete the unsubstantiated statement about our study being ‘not reliable’. As stated in the paper this was a benefit-harm analysis based on very recent systematic overviews by some of our co-authors, so it was not necessary to repeat them.


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    3. On 2014 Aug 18, David Colquhoun commented:

      NHS Choices does rather good assessments of medical headline news. I notice that they say of this study

      "While the findings of this study show promise, it is not clear whether the methods used in compiling it were systematic, so the results may not be entirely reliable."


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    4. On 2014 Aug 16, Hilda Bastian commented:

      Thanks for replying, Mangesh Thorat. I didn't review the primary studies, so hadn't picked up the error in Sutcliffe P, 2013 with respect to the Women's Health Study (Cook NR, 2013). The concern remains valid, as it applies to most of the evidence.

      I disagree, though, that the Sutcliffe review has a "major flaw," considering all studies equal irrespective of follow-up. Their analyses for duration of follow-up are front and center. And they specifically report on, and discuss, 20-year analyses on colorectal cancer, in coming to their conclusions.

      Nor are they the only group in this field to consider studies with shorter follow-up (see for example Rothwell PM, 2012). And the Physicians' Health Study (Steering Committee of the Physicians' Health Study Research Group., 1989) had 5-year follow-up.

      Many people agree with your statement that "the evidence supporting aspirin's benefits on cancer is now overwhelming." But many do not. The National Cancer Institute's recent round-up (NCI, 2014) considers perspectives on the same body of evidence. NCI highlights "mixed opinions" and "reasons for caution."

      While the potential for important net benefit from daily low-dose aspirin for more people is vitally important, I don't think the issue of harms of longterm use should be too easily dismissed. People who have common conditions that are potentially affected by taking aspirin daily (like asthma (Morales DR, 2014)), or at high risk of developing ARMD from mid-life, or whose concomitant medication use may be a relevant consideration (such as with arthritis (Colebatch AN, 2011)) might well want less uncertainty about what this means for them.

      Given the differing interpretations of this body of evidence, the findings of the US Preventive Services Task Force review, expected this year, will be interesting (NCI, 2014).


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    5. On 2014 Aug 15, Mangesh Thorat commented:

      We thank Hilda Bastian for her comment, our response to the points raised is given below:

      Sutcliffe P, 2013's systematic review is not discussed in Cuzick J, 2015 because we believe that it has a major flaw; it considered all reviews to be equal irrespective of the length of follow-up. For example, the review by Seshasai SR, 2012 that failed to show any cancer benefit had a follow-up of only 6 years. As it takes 5 years for aspirin’s beneficial effects on mortality to appear, inclusion of such data by Sutcliffe P, 2013 resulted in underestimation of beneficial effects on cancer. The updated results of WHS (Cook NR, 2013), which showed 42% reduction in CRC incidence were published almost at the same time as Sutcliffe P, 2013, and therefore were not included in this review. Sutcliffe P, 2013 based their interpretation on earlier WHS results (Cook NR, 2005), which did not show any reduction in CRC.

      Sutcliffe P, 2013 also were under wrong impression that all the primary studies and meta-analyses for benefit "assessed reduction in cancer incidence and mortality retrospectively through re-analysis of RCTs of aspirin for primary prevention of CVD." Cancer incidence and mortality is one of the primary endpoints in the WHS (Cook NR, 2013). The importance of WHS lies in the fact that it not only confirmed the benefit in cancer as a primary endpoint, even with alternate day low dose, but also confirmed that there is a long lead time and a prolonged carry-over benefit. This is where the recent WHS publication (Cook NR, 2013) differs from results published earlier (Cook NR, 2005).

      We also disagree with the statement that “uncertainty around the cancer estimates remains high”, a very large body of evidence from observational studies (Bosetti C, 2012; Algra AM, 2012) is consistent with the findings from RCTs and should not be ignored as done in Sutcliffe P, 2013. The evidence supporting aspirin’s benefits on cancer is now overwhelming with over 200 published studies and those with adequate follow up showing very consistent evidence for a reduced incidence and mortality of three major digestive track cancers – colon, stomach and oesophagus.

      It is clear from the evidence that the harms associated with aspirin (and the cardiovascular benefits) begin at the time of use and cease with stoppage of drug use. However, cancer benefits have a lead time before becoming apparent, but these continue for a long period after stopping drug use; a long carry-over effect as seen with other preventive drugs like tamoxifen. With this understanding, mere pooling of data from meta-analyses and trials with variable treatment durations and variable post-treatment follow-up to assess benefit and harms, as Sutcliffe P, 2013 have done is not a reliable method for assessing the impact of aspirin. This is primarily where our work and therefore the results differ.

      In addition, we have modelled benefits and harms of aspirin for the average risk population using actual event rates in the general population to give estimates of the impact of aspirin specifically for this group, which is the major focus of our work.

      We accept that the question of aspirin’s impact on ARMD is unresolved, but ARMD is uncommon (National Eye Institute) below 70 years of age, which again is the group on which we have focussed our attention.


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    6. On 2014 Aug 10, Hilda Bastian commented:

      These authors (Cuzick J, 2015) come to a more positive conclusion about the state of the evidence on routine aspirin use and cancer prevention than do Sutcliffe P, 2013 (also reported at Sutcliffe P, 2013).

      Sutcliffe P, 2013 undertook a thorough and well-reported systematic review of the evidence, based on previous systematic reviews, the primary studies in them, and the relevant RCTs published post-2008, re-analyzing the primary study data. They took into account the same individual patient data and other meta-analyses on which Cuzick J, 2015's interpretation of benefit rely. (Sutcliffe P, 2013's systematic review is not discussed in Cuzick J, 2015.)

      The main data included in Cuzick J, 2015 but unavailable to Sutcliffe P, 2013 appear to be an analysis of harms (where insufficient detail on the sources or selection process have been published), and a long-term follow-up report from the Women's Health Study (Cook NR, 2013). However, as Cook NR, 2013 shows a broadly similar outcome to the <10 year results (no effect on total cancers, but an effect on colorectal cancer only), this does not appear to account for the difference in interpretation of the state of the evidence by these two groups.

      The main data relied on in Sutcliffe P, 2013 that differ to those in key analyses of Cuzick J, 2015 are the Physicians' Health Study (Steering Committee of the Physicians' Health Study Research Group., 1989) and the Women's Health Study (Ridker PM, 2005). These are of long-term aspirin use on alternate days, rather than daily. These two studies include around 62,000 people, and Sutcliffe P, 2013's analyses show they dominate several calculations.

      Sutcliffe P, 2013 point to a critical issue: all the primary studies and meta-analyses for benefit "assessed reduction in cancer incidence and mortality retrospectively through re-analysis of RCTs of aspirin for primary prevention of CVD." They conclude that the uncertainty around the cancer estimates remains high, and the "long term all-cause mortality data does not provide a compelling case for aspirin protection against CVD and cancer mortality."

      With further trials underway, the picture may become clearer in the next few years. While previous trials and analyses address the major harms associated with long-term daily aspirin use (hemorrhagic stroke and gastrointestinal bleeding), many people considering this intervention may also be concerned about additional outcomes. For example, the still-unresolved question of any potential impact on neovascular age-related macular degeneration (Klein BE, 2012, Liew G, 2013, Christen WG, 2014).


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    1. On 2016 May 10, Morten Oksvold commented:

      Please pay attention to the following report from ORI (Office of Research Integrity) before reading this article:

      https://ori.hhs.gov/content/case-summary-pastorino-john-g


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    1. On 2014 Aug 13, Amanda Capes-Davis commented:

      This study looks at laryngeal carcinoma, using patient tissue and a cell line model. Please be aware that the cell line used here, HEp-2, is not from laryngeal carcinoma. HEp-2 is cross-contaminated with HeLa and is actually cervical adenocarcinoma. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2014 Aug 28, Mohammad Rostami Nejad commented:

      I read with interest the paper by Rahmati et al. entitle” Correlation of Tissue Transglutaminase Antibody with Duodenal Histologic Marsh Grading” which retrospectively reviewed hospital files of 159 patients with available tTG titer and pathology reports in the gastrointestinal clinic of Firoozgar Hospital, Tehran, Iran. They reported that the mean tTG titers was significantly higher in patients with Marsh III (a-c) and more than 9 folds higher than the kit’s cut-off value. In their conclusion they said that small intestinal biopsy should always be considered in case of high clinical suspicion, regardless of the results of serologic testing and I personally not agree with this statement. New guidelines confirmed that celiac disease diagnosis in children can be made on the basis of clinical signs, serology and genetics without the need of biopsy. Therefore, in my opinion HLA typing is useful tool for this matter and can be used as diagnosis tool for celiac disease and we can avoid invasive procedures like endoscopy in these cases.


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    1. On 2014 Aug 10, Ryan Radecki commented:

      Post-publication commentary:

      "Bizarrely Alarmist Pediatric URI Study"

      In our new Gawker and Buzzfeed-fueled, short-attention span reality, attention-grabbing headlines are essential. So, let me come up with the modern headline for news coverage of this latest article, published in Pediatrics: “Is your child's next cold a killer?”

      Seriously, as covered by Medscape (subscription required): “As many as 1 in 3 children seeking treatment in the emergency department for influenza-like illnesses (ILI) at the peak of influenza season are at high risk of suffering severe complications, such as pneumonia.”

      But, that’s hardly the case....

      http://www.emlitofnote.com/2014/08/bizarrely-alarmist-pediatric-uri-study.html


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    1. On 2015 Mar 15, David Simpson commented:

      Mass spectrometry-based proteomics dataset deposited with the ProteomeXchange Consortium (http://proteomecentral.proteomexchange.org) via the PRIDE partner repository with dataset identifier PXD001528; DOI: 10.6019/PXD001528 (http://dx.doi.org/10.6019/PXD001528).


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    1. On 2014 Aug 12, Jacob Puliyel commented:

      I congratulate the authors of this analysis. However their analysis begs more questions than it answers.

      They found that there were 581 cases of ultrasound diagnosed intussusception per 100,000 child years, during the Rotavirus trial, which works out to be 1 intussusception in every 172 children, each year, or 1 intussusception for every 86 children who were followed up for 2 years in the study (approximately - not counting 6 weeks before vaccination).

      Bhandari et al Bhandari N, 2014 have reported that 40 babies have to be vaccinated to prevent one severe rotavirus gastroenteritis episode (NNT = 40) in the 2 year of study.

      The analysis by Jehangir et al Jehangir S, 2014 of data from the Rotavirus vaccine trial showed that 1 in every 86 babies in the trial: 1) developed symptoms and signs of intussusception confirmed by a study pediatrician (namely pass blood in stools, or have continuous vomiting, abdominal distension or abdominal lump) and 2) had the diagnosis of intussusception confirmed on ultra sound.

      About half the cases resolved spontaneously. In field conditions, the other half will need urgent radiographic reduction or surgery and if these are not available (in remote villages where the vaccine will be administered), mortality is near 100%

      Jehangir and colleagues report intussusception in the study sample, without differentiating the babies who received the study drug (rotavirus vaccine) from those who received placebo. This differentiation is crucial because the rate of intussusception in the controls can be assumed to be the natural rate of intussusception using the surveillance methods described in the study.

      As the study has now been analysed after unmasking the vaccine recipients, this data on how many among the trial drug recipients and how many among the placebo recipients developed (ultrasound proven)intussusception, should be provided on the PubMed Commons. From this we can determine the NNT for intussusception (numbers of babies that need to be vaccinated to cause intussusception in 1 child) The authors need to publish data on the number of ultrasound diagnosed intussusception per 100,000 child years among those who received rotavirus vaccine and the corresponding figure for placebo recipients.

      Instead of this comparison, the authors do a retrospective analysis of data on intussusception treated at their tertiary referral hospital, between 1 January 2010 and 31 August 2013.

      Only babies who had intussusception that needed surgical or radiological treatment and which was confirmed on ultrasound examination, were included.

      Thus only cases qualifying as intussusception at Level 1 diagnostic certainty, were included and all those whose intussusception resolved spontaneously (without medical intervention) were excluded from the retrospective study.

      Under these circumstances it is meaningless to assert that all the babies selected for analysis in the retrospective study needed some intervention but only about 44% of those that were identified in the rotavirus vaccine-trial-active-surveillance, needed intervention.

      The authors then go on to conclude that, as 56% of babies with ultrasound diagnosed intussusception in the vaccine trial recovered spontaneously, active surveillance is not a good method to detect adverse events following immunization, and that sentinel hospital based surveillance (for post marketing surveillance after rotavirus vaccine introduction) was better.

      The rationale for this conclusion is difficult to fathom. Children who come to tertiary centers (and sentinel surveillance hospitals) with intussusception usually survive. It is the babies in remote areas, far away from roads and transport who die untreated and undiagnosed after intussusception.

      The sentinel surveillance will have no record of these cases of intussusception or deaths. Their deaths will not even be counted using the WHO recommended strategy of sentinel hospital based surveillance. That is the big tragedy.


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    1. On 2014 Aug 12, Jacob Puliyel commented:

      I read with interest this paper that describes efficacy and safety of the 116E rotavirus vaccine in the 2nd year of the trial. The results for the first year were published earlier in June 2014 Bhandari N, 2014. The authors need to be congratulated for this study.

      However some of the data appears incongruous. According to the clinical trial registry http://clinicaltrials.gov/show/NCT01305109 one of the secondary outcome measures was to be "safety of ORV 116E for intussusception events [Time Frame: Up to 2 years of age] Safety of ORV 116E for intussusception events in comparison to a placebo will be assessed in all subjects, from day of 1st dose till the age of 2 years (24 months) + up to 14 days". The term used here is 'intussusception events' not specifically only cases with Level 1 certainty.

      The multicenter trial was conducted in 3 centers at Delhi, Pune and Vellore. The study was done in 6799 infants of whom 4532 received the 116E rotavirus vaccine and 2267 received placebo. In the Vellore limb of the study 1000 received the vaccine and 500 were given placebo.

      Bhandari N, 2014 reports that 8 babies developed intussusception (intussusception by Brighton Level 1 criteria) during the 2 year follow up . However Jehangir et al, in the same issue of the journal Vaccine Jehangir S, 2014 report that there were 16 cases of intussusception (diagnosed on ultrasound) in the 1500 infants followed up at Vellore. 7 of these required radiological reduction meeting Brighton criteria level 1.

      It seems unlikely that there were 16 children with intussusception in Vellore center (7 meeting level 1 criteria) and there were only 11 cases in the entire trial. This would mean that there were 7 cases (meeting level 1 criteria) in Vellore among 1500 children studied and only 4 case among the 5041 children at Delhi and Pune. In view of this, I will request the authors to report in the PubMed Commons how many babies in the two group (vaccinated and placebo group) had intussusception (any level of diagnostic certainty by Brighton criteria ) and how many had Level 1, Level 2 and Level 3 certainty.


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    1. On 2014 Aug 15, Jacob Puliyel commented:

      Licensing the vaccine for general use (in remote areas of India), seems impossible to justify

      I commend Dr John and colleagues for this report on the trial with the 116E Indian rotavirus vaccine. However the authors limit their discussion to comparisons with the trials of Rotarix and Rotateq which recruited some 60,000 patients each. It will be more useful to compare the 116E trial safety results with the RotaSheild vaccine trials http://www.path.org/vaccineresources/files/RotaShield_Fact_Sheet_CDC.pdf.

      RotaSheild trial

      The RotaSheild trial recruited double the numbers recruited in the present 116E study. RotaSheild was licensed after the trial involving 14,687 patients (10,054 received the rotavirus vaccine and 4,633 received placebo). In the study there was one case of intussusceptions among the 4633 receiving placebo. This suggests that the ‘normal rate of intussusception’ was approximately 2/10,000, in that population. Five cases of intussusceptions occurred among 10,054 RotaSheild vaccine recipients. Thus there were an excess of 3 cases of intussusceptions for each 10,000 children vaccinated. All the intussusceptions were among infants who received a second or a third dose of vaccine. The difference between the vaccinated and placebo recipients was not statistically significant http://www.path.org/vaccineresources/files/RotaShield_Fact_Sheet_CDC.pdf.

      116E Trial

      With the 116E vaccine trial there were 6 cases of intussusceptions in 2267 controls which works out to be 2.6 cases per 1000 placebo recipients. The ‘normal rate of intussusception’ in this study was at least 10 times higher than the RotaSheild trial (where it was 0.2 cases per 1000 placebo recipients). There were 17 cases of ultrasound confirmed intussusceptions among the 4532 given the 116E vaccine which is 3.75 cases per 1000 babies vaccinated. The comparative figure for the RotaShield study was 0.5 cases/1000. In the 116E trial there was an excess of 1 case of intussusceptions for every 1000 children vaccinated with the rotavirus vaccine (compared to the RotaSheild trial where there were 3 excess intussusceptions per 10,000 vaccinated). RotaSheild vaccine was withdrawn after licensing, on account of unacceptable risk of intussusception. The risk of intussusception in the 116E trial was three times higher than with the RotaSheild trial. We are told that in the 116E trial, 50% intussusceptions diagnosed by ultrasound, resolved spontaneously John J, 2014. In the remaining 50% there is need for urgent treatment by a radiologist or pediatric surgeon. In remote parts of India, without motorable roads, let alone radiologists and pediatric surgeons, mortality will be near 100% http://emedicine.medscape.com/article/930708-overview. Such specialized care (radiological or surgical reduction of intussusception) is not available in vast swathes of India and we can assume vaccinated babies would die at home passing blood and mucus in the stools and it will be presumed they had died of dysentery and sepsis rather than intussusception caused by the vaccine.

      Intussusception risks compared to diarrhea deaths avoided

      Assuming only 50% ultrasound diagnosed intussusceptions need urgent treatment John J, 2014 we can assume that one child in 2000 vaccinated babies will develop this life threatening condition. The possible harm in remote areas (deaths from intussusceptions 1/2000) is not offset by benefits (diarrhea deaths avoided using the 116E vaccine).

      In the first two years after vaccination, there number of infants that needed to be immunized to prevent one episode of rotavirus diarrhea of any severity was 21 Bhandari N, 2014. Assuming mortality from rotavirus diarrhea to be 1% in the first 2 years of life with community management Lal S, 1994 Kosek M, 2003 2100 babies will have to be vaccinated to prevent one death from diarrhea in the first 2 years of life.

      When 2100 babies are vaccinated to prevent that 1 death from rotavirus diarrhea - 1 child will have intussusceptions and die in remote areas of the country. This is why, given the limited evidence of this 116E trial, licensing the vaccine for general use (in remote areas of India), seems impossible to justify.


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    1. On 2016 Jul 21, Jacob H. Hanna commented:

      Theunissen et al. Cell Stem Cell 2014 reported absolute failure to detect human naïve PSC derived cell integration in chimeric mouse embryos obtained following micro-injection into mouse blastocysts, as was reported for the first time by our group (Gafni et al. Nature 2013). However, the authors failed to discuss that imaging and cell detection methods applied by Theunissen et al. Cell Stem Cell 2014 were (and still) not at par with those applied by Gafni et al. Nature 2013.

      Regardless, we find it important to alert the readers that Theunissen and Jaenisch have now revised (de facto, retracted) their previous negative results, and are able to detect naïve human PSC derived cells in mouse embryos at more than 0.5-2% of embryos obtained (Theunissen et al. Cell Stem Cell 2016 - Figure 7) Theunissen TW, 2016 < http://www.cell.com/cell-stem-cell/fulltext/S1934-5909(16)30161-8 >. They now apply GFP and RFP flourescence detection and PCR based assays for Mitochondrial DNA, which were applied by the same group to elegantly claim contribution of human neural crest cells into mouse embryos (albeit at low efficiency (Cohen et al. PNAS 2016 Cohen MA, 2016).

      While the authors of the latter recent paper avoided conducting advanced imaging and/or histology sectioning on such obtained embryos, we also note that the 0.5-2% reported efficiency is remarkable considering that the 5i/LA (or 4i/LA) naïve human cells used lack epigenetic imprinting (due to aberrant near-complete loss of DNMT1 protein that is not seen in mouse naive ESCs!! http://imgur.com/M6FeaTs ) and are chromosomally abnormal. The latter features are well known inhibitors for chimera formation even when attempting to conduct same species chimera assay with mouse naïve PSCs.

      Jacob (Yaqub) Hanna M.D. Ph.D.

      Department of Molecular Genetics (Mayer Bldg. Rm.005)

      Weizmann Institute of Science | 234 Herzl St, Rehovot 7610001, Israel

      Email: jacob.hanna at weizmann.ac.il

      Lab website: http://hannalabweb.weizmann.ac.il/

      Twitter: @Jacob_Hanna


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    2. On 2016 Jul 14, Jacob H. Hanna commented:

      None


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    1. On 2016 Jan 21, Rupert Collins commented:

      The authors may wish to revise the identification of this fish. I blasted the COI and CYTB sequences, and both were from the goldfish (Carassius auratus), and not from Piaractus brachypomus. http://www.ncbi.nlm.nih.gov/nuccore/KJ993871


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    1. On 2014 Oct 29, Benoit Kornmann commented:

      The unfolded protein response (UPR) is a conserved pathway that senses stress in the endoplasmic reticulum (ER) and responds to it by eliciting a transcriptional response. Mechanistically, when the stress sensor IRE1 is activated by the accumulation of unfolded proteins in the ER, its cytosolic RNAse domain cleaves the messenger of a transcription factor (Xbp1 in mammals, Hac1 in yeast) at two precise positions, removing an inhibitory intron. The 5' and the 3' parts of the messenger are then re-ligated together, to encode a functional transcription factor that takes part in the response. While the ligase involved in the last processing step was known in yeast, it evaded identification for years in mammals.

      Here, the mammalian ligase is identified using a clever trick. A synthetic construct consisting of a Cre recombinase fused to Xbp1 is not expressed in normal conditions, but upon ER stress, Xbp1 is spliced and Cre recombinase is produced. The induction of the recombinase can be easily monitored using a Cre-induced proapoptotic factor, which kills the cells. Using this synthetic circuit, the authors screen a lentiviral RNA interference (RNAi) library and identify hits that fail to induce Cre upon acute ER stress, by simply scoring for survival. They identify the ligase RtcB, which, as with the yeast UPR ligase Trl1, is also involved in tRNA splicing.


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    1. On 2014 Nov 26, Marc Girard commented:

      By the distance between what it demonstrates and what it claims, this paper (as well as the preceding IOM report this one is supposed to update) illustrates that the issue of vaccines safety is still a matter of serious concern for anyone endowed with a minimum of expertise in drug safety or pharmacoepidemiology.

      To start with methodological consistency, one may wonder why the McHarm instrument used by the authors to assess the quality of the reviewed studies was not published in a peer-reviewed journal (the internet link given by the authors [their ref. 7] being not accessible) whereas the only investigations they included had to be published (in contrast with Cochrane reviews which, inasmuch as possible, also take into account unpublished investigations). This inconsistency in the authors’ way of referencing sources exposes their review to a number of biases which are well known in general, but reach unparalleled levels as far as vaccines are concerned. To take just one example, the Ascherio et al.’s study, which suggested a lack of neurotoxicity with hepatitis B vaccination, was triumphantly published in The New England Journal of Medicine (2001;344:327-32) (despite its worrying biases, some of them detailed in further correspondence) with an accompanying editorial celebrating the study as a milestone, whereas, in spite of the professional fame of its authors and of its intrinsic quality, a later study on the same subject by Hernan et al., which suggested opposite conclusions, was first rejected by The NEJM, The Lancet, The BMJ (personal communication), before being published in Neurology (2004;63:838-42) with an accompanying editorial contending that nothing significant had changed regarding the safety of this immunization: as a matter of fact, Hernan was a co-writer of both studies… Another example of selective assessment, extracted from Maglione et al.’s paper itself: it remains unclear why the study by Gallagher and Goodman (which suggests a link between hepatitis B vaccine and autism) would display “high risk of bias and low quality”, whereas the “protective effect [of some vaccines] against acute lymphoblastic leukemia” does not deserve the slightest word of caution… Dozens of additional examples of publication biases could be cited: this is the personal experience of anyone working in the field of vaccines that positive results or enthusiastic reviews are far more easily published than negative investigations or critical comments. Finally and as a number of respected authors have already emphasized, a major part of vaccines studies are performed or supported by manufacturers or governmental agencies responsible for previous recommendations, a situation which clearly maximizes conflicts of interests.

      Regarding now experimental designs in vaccine studies, the following list of methodological defects is concerned with safety assessments (but could be easily extended if efficacy issues were also concerned).

      i) During development, use of false placebos as comparators (i.e. not devoid of pharmacological effects: adjuvants, other vaccines) is a frequent practice.

      ii) Compared to the supposed duration of the beneficial immunological effects of the tested vaccines, the duration of the safety studies aimed at assessing a potential for delayed immunological hazards is often ridiculously short.

      iii) Required on a standard regulatory basis with any new pharmacological entities, the interactions studies are weak, scarce, if not nonexistent with vaccines, whereas most of them are now administered as combinations.

      iv) Likewise, the dose-ranging studies are generally defective, accounting for impressive changes in the booster recommendations once the vaccine is on the market, which would be inconceivable for any other drug.

      Overall and as far as safety issues are concerned, Cochrane reviewers (e.g. in their reviews of flu vaccines) frequently identify blatant weaknesses in available studies which, apparently, are beyond of the reach of the McHarm instrument… On the contrary, Maglione et al. expressed frequent reservations about the “the strength of evidence” suggesting potential safety issues, but none about the power of the reviewed studies to effectively grasp evidence of vaccine hazards… Likewise, the authors are clearly not concerned with the tremendous tendency of vaccine studies (pre- or post-marketing) to underreport adverse events: experience suggests that physicians have a worrying reluctance to accept that vaccines might have adverse effects and, besides their indisputable tendency to brush aside any such suggestions from their patients, they do not hesitate to present as reassuring that “immunizations are up to date” when confronted with an unexplained disease, without even considering that these immunizations could have triggered the disease in question… Another illustration of the same bias: when reassuring, VAERS data are unchallenged, whereas the shortcomings of the system are immediately pointed out each time they may suggest a safety problem…

      Maglione et al.’s review is regrettably silent on two crucial issues of the continuous extension of immunizations against trivial diseases:

      i) maybe acceptable for one vaccination against a severe disease, the autoimmune risk related to the administration of foreign material increases arithmetically when vaccinations are multiplied beyond any sound limit;

      ii) extended immunizations greatly alters the natural ecology of a number of infectious diseases (e.g. measles), a situation the assessment of which would be far more complex than the basic inventory of straightforward side-effects which, as mentioned above, is already severely defective from a methodological point of view: no reason to believe that vaccine promoters are better in complex assessments than in trivial ones…

      As is easy to document, the never-ending extension of immunizations against anything is based upon the dramatization of anecdotic stories, sometimes tragic but fairly rare or even exceptional at a community scale. Yet, experience of drug assessment suggests that below frequencies of, at best, 1-2% of exposed patients, clinical trials fail to identify drug side-effects with a minimum of reliability (the statistical power of postmarketing surveillance being even lower by far). In a country like the USA, this detection threshold is consistent with a shadow area on iatrogenic risk of about 40,000-80,000 persons per vaccine for each vaccinated class of age: it should be obvious that risk-taking of such a size is simply disproportionate to the potential benefits of reducing the morbidity of trivial diseases (even taking into account the natural tendency of vaccine promoters to exaggerate the efficacy of immunizations…). The stubborn obfuscation of this evident arithmetical imbalance by health professionals or governmental agencies suggests that there is something rotten in the kingdom of immunization…

      Marc GIRARD, MSc, MD


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    1. On 2014 Aug 04, Paul Brookes commented:

      This paper addresses a very important point... namely, one of the proposed mechanisms by which ischemic preconditioning (IPC) is thought to bring about cardioprotection. It has been hypothesized that increased leakiness of the mitochondrial membrane to protons may lead to a lowering of ROS generation. We provided some evidence to support increased H+ leak in IPC in 2006 Nadtochiy SM, 2006. Unfortunately, it's not immediately clear to me exactly how the authors measured H+ leak in this study, and also whether their ROS measurements were performed correctly.

      First proton leak: The normal way this is determined is to make simultaneous measurements of membrane potential and respiration in a single chamber equipped with an oxygen electrode and another electrode sensitive to a lipophilic cation such as TPP+. The authors are to be commended on their choice to use a TPP+ electrode, which instantly makes this paper more quantitative than others using qualitative fluorescent probes such as TMRE. They measured membrane potential (as reported in Figure 3) using succinate as a substrate for complex II, with rotenone to inhibit complex I. All good so far. However, normally oligomycin is added to inhibit the ATP synthase as a potential source of leak. In addition nigericin is added to equilibrate K+/H+ and thus ensure the potential is a measure of protonmotive force. As such, the potential measured here was not in a true state 4 condition which is typically required for quantitation of proton leak.

      After describing membrane potential measurements, the methods section describes respiration and H+ leak methodology. It appears oligomycin was added this time (good!), but then something very odd happens... it is stated that "H+ leak was measured as the state 2 respiration rate required to maintain membrane potential at -150mV". Nowhere is it stated how that value of 150mV was arrived at. Normally, when doing these measurements, you set the mitochondria in state 4 (succinate, rotenone, oligomycin, nigericin), and then titrate the activity of the respiratory chain with an inhibitor such as malonate. Step-wise titration then gives you a series of membrane potential and respiration traces, a curve, from which the leak rate at any given potential can be read off. The question is, if such curves were made, how were they made (no mention of malonate anywhere), and why aren't they shown in the paper? The scary alternative explanation may be that they "measured" leak by imposing the 150mV membrane potential by titrating in uncoupler. This is incorrect - you can't add something that changes the leak as a way of measuring the leak. The other odd thing is that the average baseline membrane potential in the IR group barely above 150mV, so some replicates in that group must have had a potential value below 150mV to begin with. How did they authors get those mito's UP to 150mV for the leak measurement? Overall, it would be a whole lot better if they just showed the full leak curves.

      What about ROS? The problems here are two-fold. First it appears that SOD was not added to the incubations to scavenge any stray superoxide and turn it into H2O2 for the assay to pick up. Second, the calibration of the assay was performed incorrectly. It is stated in the methods that the signal was calibrated by "adding known concentrations of H2O2 to buffer solution containing horseradish peroxidase and Amplex-Red" The problem is, it is necessary to calibrate in the presence of mitochondria, so the signal you measure with the calibrating H2O2 is under the same condition as the measurement itself. The way this is commonly done is to just add a bolus of H2O2 at the end of each run. This has the advantage of making every run internally calibrated, which cuts down on noise (this is a very noisy assay). The outcome here is a bit odd... the values of H2O2 generation are in the range of 10-40 nM/min/mg protein. Ignoring the odd units (rates of things should be expressed in moles not Molar), let's assume they meant to write nmols/min/mg - that would put their rates about 1500-fold greater than typical for these conditions (e.g.Chen Q, 2003).

      So, TL/DR - good ideas, but more info' is needed on the proton leak method, and the ROS numbers are just wild. Also, lest anyone think I'm attacking this work because I happen to be one of the people who originally proposed proton leak --> lower ROS --> protection in IR injury, that's not the case. In-fact, my lab' is now pursuing a completely different downstream signaling mechanism, as a mediator of the protective effects of mitochondrial uncoupling, so if the results of this paper are true, my life just got a whole lot easier! I just want to be sure before I start citing it.


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    1. On 2014 Sep 09, Vahid Rakhshan commented:

      Reply to the author’s response: Statistical errors in a recent article: Sella Turcica in patients with Type 1 diabetes

      1. The authors kindly stated in the authors’ reply that it was clearly written in the 4th paragraph of Methods that how the subjects were matched: "This was clearly defined in the 4th paragraph of Material and Methods section. In addition, the need to match the groups according to bone age, not the chronological age was discussed briefly in Discussion (paragraph 3, page 183) with supporting references." (A) I re-checked the 4th paragraph and there was no indication of criteria for matching. The authors had indeed talked about grouping the patients according to the bone age, in the 4th paragraph ("that were equally distributed into subgroups according to bone age and sex."), but that was not something about "matching" the patients. (B) Moreover, there was no mention of the chronological age in that 4th paragraph of the Methods section. However, this factor is used for correlating the two groups, according to the Results and Discussion. (C) Furthermore, in the same Methods sentence that had stated that bone age was used for grouping ("that were equally distributed into subgroups according to bone age and sex."), sex was mentioned as a grouping factor as well. So if that quoted sentence implies that bone age was a matching factor, should we consider sex as a matching criterion as well? The above-quoted sentence from the 4th paragraph of the Methods is actually the criteria for dividing the sample into subgroups. However, the authors are referring to it (in the authors’ reply) as something about matching. (D) Besides, I had noticed the comparisons and correlations of groups regarding bone ages, in the pages 182 and 183, but since those factors were not pre-defined as criteria for matching, those comparisons and the authors’ accompanying correlations could not indicate a matching between the groups to the reader.

      2. I appreciate the authors’ point #2. They kindly clarified the authors’ method.

      3. The authors have stated in the authors’ reply that they had tested both the whole sample and each subgroup regarding the normality... First that the authors’ article stated n > 50 for the normality test. However, the authors’ subgroups were much smaller than this. So n > 50 could not relate to subgroups of n = 19. Therefore, either the statement "n > 50" was incorrect, or they had not tested for normality in the subgroups. Moreover, normality should not be tested in the whole sample. It is completely incorrect. Besides, they did not state why they had used two different normality tests?

      4. There is nothing wrong with doing a pairwise comparison, and I did not say pairwise comparisons are bad, in my original letter. However doing a pairwise comparison without an ANOVA is statistical malpractice (when the ANOVA is necessary) and bad. It might have the following problems: (1) The absence of ANOVA disallows to assess the interactions. (2) Without an ANOVA design first, we do not know if any post hoc (or pairwise) comparisons are necessary or not, in the first place. If the ANOVA is non-significant, then performing the pairwise comparisons is simply moot (if we disregard the family-wise error introduced by the unnecessary statistical analyses). So this was why I was emphasizing on performing an ANOVA before doing the pairwise comparisons.

      5. The authors kindly stated " In our manuscript, "matched" means "constructing two groups whose data would be comparable with each other"." ... "The data of these groups are independent from each other and the presence of one group cannot alter the data of the other. " (A) Please note that "matched" has its own globally accepted definition that is to select groups with similarities in certain aspects. So using a personal definition for this word is not a healthy practice. (B) Moreover, the statement "constructing two groups whose data would be comparable with each other" implies (by the word "comparable") that there were actually similarities between the two groups, and thus some sort of matching had been actually performed. This again reveals that the two groups were not independent. (C) Furthermore, the Results and the Discussion (pages 182 and 183) clearly indicate that the two groups were correlated with each other according to the chronological and bone age: Page 182: "For both groups, the chronologic and bone ages of the subjects were correlated to each other" Page 183: "The control group, on the other hand, was created from skeletal Class I patients with no systemic diseases and whose chronologic and bone ages were correlated." (D) This evidence completely suffices to invalidate the use of ANY independent-samples test. Correlated groups CANNOT be independent. How "the presence of one group cannot alter the data of the other" when the authors had themselves selected the control group in a way that they were correlated to diabetic patients in terms of chronological and bone age? The control group was already altered in a way that it could be correlated to the diabetic patients.

      6. The authors have kindly re-stated that they had used the Bonferroni correction method. I had already seen the authors’ similar statement in the authors’ paper, but had not found any evidence supporting the authors’ statement. Please note that the Bonferroni correction is simply dividing the alpha by the number of pairwise comparisons in each family of tests. So we would expect to see alphas below 0.05 (for example 0.013 etc. depending on the number of pairwise comparisons). In that case, if the alpha had been corrected using the Bonferroni method to something like 0.008, and the P value had become P = 0.04, the P was still Non-Significant. However, throughout the text, and in the tables, only P values above the alpha = 0.05 had been considered as non-significant. This indicated that no Bonferroni had been used to adjust the alpha. (the alpha had not been adjusted in the first place).

      7. I much appreciate the authors’ correction and clarification.

      Many thanks for the readers' and authors' time.

      With kindest regards,

      Vahid Rakhshan


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    2. On 2014 Sep 09, Vahid Rakhshan commented:

      None


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    1. On 2014 Sep 03, Tzevat Tefik commented:

      Instead of "P-30-U-N PCNL"I would prefer "P-U-N PNL<sup>+30"</sup>


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    1. On 2016 May 23, Heidi Schulz commented:

      Four of the five BEST1 variants published to be novel had been published before (p.Leu294Phe, p.Phe84Val, p.Gly83Asp, p.Trp93Arg, p.Trp309Arg).


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    1. On 2016 Feb 22, Daniel Corcos commented:

      Actually, it is possible to estimate the relative risk associated to mammography by comparing the incidence of cancer in women with no exposure (whose age differ from women with exposure) to that of a BRCA carrier recent birth cohort (born after 1958) in figure 3 of Gabai-Kapara et al. It is also possible to use the data on interval breast cancer after negative mammography, showing that BC incidence is divided by more than three within two years following negative mammography (Bucchi et al., 2008). Both results suggest that figure 1 and 2 of Giannakeas et al. indicate a doubling of cancer incidence as a consequence of mammography. In other terms, these results suggest that a woman carrying a BRCA1 or BRCA2 mutation has a reasonable chance of not developing cancer if she has no mammography, and a very small chance to be spared if she has repeated mammography screening.

      References

      Gabai-Kapara et al; http://www.ncbi.nlm.nih.gov/pubmed/25192939

      Bucchi et al. http://www.ncbi.nlm.nih.gov/pubmed/18416953


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    2. On 2016 Feb 08, Daniel Corcos commented:

      Whether mammography screening increases the risk of breast cancer in women with DNA repair defect is an important question. In this paper, Giannakeas et al. found no difference in cancer incidence in women with previous mammography screening as compared to women with no prior irradiation. Negative mammography identify a population with a lower risk, since women with breast cancer are not part of the study. In the case of colon cancer, people with previous negative colonoscopy have a strongly reduced risk as compared to people with no previous colonoscopy (Brenner et al., 2011). Similarly it would be expected that women with negative mammography have a lower cancer incidence as compared to women with no previous mammography. Thus, Giannakeas et al. result suggests that mammography increases the risk of developing breast cancer in mutation carriers. http://www.ncbi.nlm.nih.gov/pubmed/21876077


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    1. On 2014 Aug 02, Hilda Bastian commented:

      While safer driving by adolescents is a critically important issue - and further research in this area is definitely needed, the authors' conclusions about the effects of this intervention are overly positive.

      The parent in these trials was overwhelmingly the mother (over 80%), mostly college-educated - and non-white families appear to have been under-represented. The participants responded to hearing about the trial rather than being actively recruited, and so were particularly highly motivated - and the trial couldn't reach its recruitment goal. Further, 16% of the intervention group were lost to follow-up at the primary outcome measurement point (compared with 6% in the control group).

      Even with this highly motivated group in a trial setting, of an intervention more intensive than a large-scale program could be (Ramirez M, 2013), and with outcomes based solely on the adolescents' reports, pre-specified primary outcomes (trial registration record) did not achieve statistical significance. While the authors fairly attribute this to low recruitment making the trial under-powered, it isn't very encouraging. As the authors point out, there's no strong effect apparent here.

      Presenting the adolescents' self-reported Risky Driving Score results as risk reduction percentages in the abstract risks giving people an exaggerated impression of effectiveness. The range of possible score isn't very wide, so even a small difference can be a substantial percentage. It would have been good if more details about the score were provided, given that it's a primary outcome measure and it was a trial-specific adaptation of an existing score.

      It's great to see this trial published, even though it didn't meet its goals. But I don't agree with the authors' conclusion that statistical significance levels should be dropped low, in effect, because proven interventions are needed. The interventions that people would use need to make a real difference. As the authors point out, there is evidence that parents can make a difference to their adolescents' behaviors - to their list, I'd add influencing smoking (Thomas RE, 2007). But parents need to know where they could make the best effort, given the other options like Parent-Teen Driving Agreements (Zakrajsek JS, 2013) - or discouraging getting a license early (Ian R, 2001).

      The authors indicate that future research will integrate more objective data, which presumably refers to the unreported data from 2010 for driving citations and crashes in this trial. That will be vital to put this self-reported data on surrogate outcomes in perspective. Access for others to the intervention materials may be important for others in the field (Glasziou P, 2010).


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    1. On 2014 Aug 27, Ryan Radecki commented:

      Post-publication commentary:

      "Nitric Oxide Supplies No Miracles in Sepsis"

      An interesting context to end-organ dysfunction in sepsis stems from microcirculatory dysfunction, secondary to endothelial activation and vascular disruption as part of the inflammatory cascade. Even though abnormal vasoconstriction in sepsis may be pharmacologically ameliorated, microcirculatory perfusion remains impaired....

      http://www.emlitofnote.com/2014/08/nitric-oxide-supplies-no-miracles-in.html


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    1. On 2014 Aug 17, Airton Stein commented:

      This issue highlights the oral health of patients who undertook a bariatric surgery. A comprehensive care is essential for this kind of health problem.


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    1. On 2014 Sep 15, Amanda Capes-Davis commented:

      This study uses HEp-2 to investigate the role of CUGBP1 in laryngeal cancer. Please be aware that HEp-2 is known to be cross-contaminated with HeLa, which is from cervical cancer. These results do not relate to laryngeal cancer.

      Laboratories can test their cell line stocks for cross-contamination using a consensus method such as short tandem repeat (STR) profiling. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2017 Jun 15, Feng Zhang commented:

      A number of researchers have inquired about the presence of duplicate sgRNAs (same sgRNA for more than one gene) in the GeCKOv2 library (Sanjana et al., Nature Methods 2014) and non-specific sgRNAs that have additional exact matches in the genome. We would like to further clarify the design considerations for GeCKOv2 (Supplementary Methods, Sanjana et al., Nature Methods 2014).

      For the GeCKOv2 libraries we decided to take the “best” sgRNA (i.e. with the fewest off-targets) we could find for a given gene, even if in some cases our “best” sgRNA had more than one targeting location in the genome. This was done to sample as many targets as possible and minimize false negatives, since false positives that are due to an sgRNA with more than one target or off target effects can be easily eliminated in post-screen validation experiments or through a gene-based analysis that selects hits based on the consistent effect of multiple unique sgRNAs. Regardless, each candidate obtained through a GeCKO screen needs to be validated through rigorous experimentation, including testing using new guides targeting each screen hit.

      A special example are gene families with high homology, in such cases our algorithm was not able to find a unique sgRNA targeting a constitutive exon. The approach that we took was to leave in these sgRNAs to give users the greatest range of options (and potential targets) during post-screen validation experiments. For example, in the human GeCKOv2 library, there are 5,664 non-specific sgRNAs. This works out to be ~4% of all guides in the library. Those redundant sgRNAs can always be removed computationally, following a screen, to simplify data analysis. (A table of these sgRNAs and genes targeted with multiple non-specific sgRNAs is available here: [link]). In contrast, GeCKOv1 did not include as many non-specific guides and consequently only targets a smaller number of genes.

      To clarify this and help users in their analysis we previously provided the GeCKOv2 sgRNA database with information about the number of off-target target hits (e.g. [link]). We also have provided an additional sgRNA index for both human and mouse GeCKOv2 libraries that lists only unique sgRNAs such that when multiple genes are targeted all of those are listed under gene_id [link].

      The GeCKOv2 libraries have already been successfully used by many groups to generate a number of interesting biological findings (e.g. Golden et al., Nature, 2017, Erb et al., Nature, 2017; Xu et al., PNAS, 2017; Jain et al., Science, 2016; Marcaeu et al., Nature, 2016; Zhang et al., Nature, 2016; Meitinger et al., JCB, 2016; Wallace et al., PLoS One, 2016; Parnas et al., Cell, 2015; Chen et al., Cell, 2015). In addition to GeCKOv2, there are a number of alternative libraries (e.g. Wang et al., Science, 2015; Doench et al., Nat. Biotechnol., 2016; Hart et al., Cell, 2015), including libraries that were designed to avoid duplicate sgRNAs by targeting fewer genes. A list of different libraries is available on Addgene’s pooled CRISPR libraries page: [link].

      We would like to specifically thank Joey Riepsaame and Timokratis Karamitros for recently bringing this issue to our attention. We also thank the GeCKO users who contacted us through the CRISPR Genome Engineering online forum and by email for additional helpful discussions.

      Neville E. Sanjana (nsanjana at nygenome.org)

      Ophir Shalem (shalemo at email.chop.edu)

      Joey Riepsaame (joey.riepsaame at path.ox.ac.uk)

      Timokratis Karamitros (timokratis.karamitros at zoo.ox.ac.uk)

      Feng Zhang (zhang at broadinstitute.org)

      References Cited

      Chen, S., Sanjana, N.E., Zheng, K., Shalem, O., Lee, K., Shi, X., Scott, D.A., Song, J., Pan, J.Q., Weissleder, R., et al. (2015). Genome-wide CRISPR screen in a mouse model of tumor growth and metastasis. Cell 160, 1246–1260.

      Doench, J.G., Fusi, N., Sullender, M., Hegde, M., Vaimberg, E.W., Donovan, K.F., Smith, I., Tothova, Z., Wilen, C., Orchard, R., et al. (2016). Optimized sgRNA design to maximize activity and minimize off-target effects of CRISPR-Cas9. Nat. Biotechnol. 34, 184–191.

      Erb, M.A., Scott, T.G., Li, B.E., Xie, H., Paulk, J., Seo, H.-S., Souza, A., Roberts, J.M., Dastjerdi, S., Buckley, D.L., et al. (2017). Transcription control by the ENL YEATS domain in acute leukaemia. Nature 543, 270–274.

      Golden, R.J., Chen, B., Li, T., Braun, J., Manjunath, H., Chen, X., Wu, J., Schmid, V., Chang, T.-C., Kopp, F., et al. (2017). An Argonaute phosphorylation cycle promotes microRNA-mediated silencing. Nature 542, 197–202.

      Hart, T., Tong, A., Chan, K., van Leeuwen, J., Seetharaman, A., Aregger, M., Chandrashekhar, M., Hustedt, N., Seth, S., Noonan, A., et al. (2017). Evaluation and Design of Genome-wide CRISPR/Cas9 Knockout Screens. bioRxiv.

      Jain, I.H., Zazzeron, L., Goli, R., Alexa, K., Schatzman-Bone, S., Dhillon, H., Goldberger, O., Peng, J., Shalem, O., Sanjana, N.E., et al. (2016). Hypoxia as a therapy for mitochondrial disease. Science 352, 54–61.

      Marceau, C.D., Puschnik, A.S., Majzoub, K., Ooi, Y.S., Brewer, S.M., Fuchs, G., Swaminathan, K., Mata, M.A., Elias, J.E., Sarnow, P., et al. (2016). Genetic dissection of Flaviviridae host factors through genome-scale CRISPR screens. Nature 535, 159–163.

      Meitinger, F., Anzola, J.V., Kaulich, M., Richardson, A., Stender, J.D., Benner, C., Glass, C.K., Dowdy, S.F., Desai, A., Shiau, A.K., et al. (2016). 53BP1 and USP28 mediate p53 activation and G1 arrest after centrosome loss or extended mitotic duration. J. Cell Biol. 214, 155–166.

      Parnas, O., Jovanovic, M., Eisenhaure, T.M., Herbst, R.H., Dixit, A., Ye, C.J., Przybylski, D., Platt, R.J., Tirosh, I., Sanjana, N.E., et al. (2015). A Genome-wide CRISPR Screen in Primary Immune Cells to Dissect Regulatory Networks. Cell 162, 675–686.

      Sanjana, N.E., Shalem, O., and Zhang, F. (2014). Improved vectors and genome-wide libraries for CRISPR screening. Nat. Methods 11, 783–784.

      Wallace, J., Hu, R., Mosbruger, T.L., Dahlem, T.J., Stephens, W.Z., Rao, D.S., Round, J.L., and O’Connell, R.M. (2016). Genome-Wide CRISPR-Cas9 Screen Identifies MicroRNAs That Regulate Myeloid Leukemia Cell Growth. PloS One 11, e0153689.

      Wang, T., Birsoy, K., Hughes, N.W., Krupczak, K.M., Post, Y., Wei, J.J., Lander, E.S., and Sabatini, D.M. (2015). Identification and characterization of essential genes in the human genome. Science 350, 1096–1101.

      Xu, C., Qi, X., Du, X., Zou, H., Gao, F., Feng, T., Lu, H., Li, S., An, X., Zhang, L., et al. (2017). piggyBac mediates efficient in vivo CRISPR library screening for tumorigenesis in mice. Proc. Natl. Acad. Sci. U. S. A. 114, 722–727.

      Zhang, R., Miner, J.J., Gorman, M.J., Rausch, K., Ramage, H., White, J.P., Zuiani, A., Zhang, P., Fernandez, E., Zhang, Q., et al. (2016). A CRISPR screen defines a signal peptide processing pathway required by flaviviruses. Nature 535, 164–168.


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    1. On 2014 Sep 30, Ryan Radecki commented:

      Post-publication commentary:

      "For tPA, Is Delusion the Standard of Care?"

      Yet again, the tPA apologists dip into their bag of registry data in an attempt to defend tPA – and end up contradicting themselves.

      In 2009, neurologists in India published a retrospective case series examining the outcomes following tPA at their institution. Specifically, they divided up the cases between those with arterial occlusion present on CT angiogram of the cerebral vessels, and those with no demonstrated arterial occlusion. For patients with demonstrated occlusion, there were significant differences in early NIHSS improvement favoring tPA, but no long term mRS improvements. Conversely, there were 119 without occlusion present – and the early NIHSS improvement and late mRS improvement outcomes were similar. There were, however, substantial baseline differences between those receiving tPA and those who did not – and retrospective studies are confounded by many biases – but there was at least a suggestion that some stroke subtypes might not benefit from tPA....

      http://www.emlitofnote.com/2014/09/for-tpa-is-delusion-standard-of-care.html


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    1. On 2014 Aug 07, Jim Woodgett commented:

      Very thorough study on the effects of complete inactivation of GSK-3 (both isoforms) on radial migration of neurons and on dendritic morphology. The results here don't agree with previously reported role of Lkb1/STK11 on negative regulation of GSK-3 (via serine 21/9 phosphorylation). This is difficult to reconcile but may reflect the fact that such phosphorylation only partially inhibits GSK-3 (~50%) and that all compartments of GSK-3 are affected by genetic knockout verses only some that are sensitive to regulation by phosphorylation. The authors also show the effects of GSK-3 inactivation are not mediated by Wnt signalling which is typically the dominant pathway that is de-inhibited under this context and in, for example, nestin-Cre/GSK-3KO animals is one of the (but not only) primary drivers of neuronal progenitor proliferation. Together, the data indicate that the effects of these kinases on radial migration are largely insulated from the many other effects on cellular functions.

      As an aside, this paper makes great use of the embedded media of eLife although there is no direct link to the eLife manuscript from PubMed yet (http://elifesciences.org/content/3/e02663).


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    1. On 2014 Aug 04, Ryan Radecki commented:

      Post-publication commentary:

      "The tPA Cochrane Review Takes Us For Fools"

      It’s been 5 years since the last Cochrane Review synthesizing the evidence regarding tPA in acute ischemic stroke. Clearly, given such a time span, in an area of active clinical controversy, a great deal of new, important, randomized evidence has been generated!

      Or, sadly, the only new evidence available to inform practice is IST-3 – a study failing to demonstrate benefit, despite its pro-tPA flaws and biases. So, it ought not be a very exciting update, considering the 2009 version included 26 trials, and the 2014 update now includes only 27 trials. Their summary conclusion, with only additional evidence of regression to the mean, ought remain essentially the same, or even less optimistic, right?

      http://www.emlitofnote.com/2014/08/the-tpa-cochrane-review-takes-us-for.html


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    1. On 2015 Sep 01, E Schuman commented:

      Critical Flaws in Ainsley et al., “Functionally diverse dendritic mRNAs rapidly associate with ribosomes following a novel experience”, DOI: 10.1038/ncomms5510

      Submitted by: Georgi Tushev and Erin Schuman (Max Planck Institute for Brain Research, Frankfurt am Main, Germany) and Wei Chen (Max Delbruck Center, Berlin, Germany).

      http://brain.mpg.de/uploads/media/Ainsley_Rebuttal_01Sep2015.pdf

      In this paper the authors conduct a fear conditioning experiment (“novel-experience”), isolate ribosome-bound mRNA from the dendrites of mouse hippocampal neurons, conduct deep RNA sequencing and then use a machine-learning classification scheme to identify the mRNAs present in dendrites following learning. Upon close reading and re-analysis of the published data we found substantive flaws including the absence of an analyzed control group, low sequencing depth, high variability between replicas, and poor classification of genes. We discuss these issues in greater detail below.

      Absence of a completely analyzed control group. In biological experiments, the assessment of statistically significant differences between groups (e.g. control and experimental groups, drawn from a normal distribution) uses information about the variability in each group in order to estimate the likelihood that between-group differences occurred by chance. Ainsley et al. attempted to compare ribosome-bound RNA from control ("home-cage") and "novel- experience" animals, ignoring their own observations (see Ainsley et al Fig. S2) that the variation among the biological replicates within each group is as large as the variation between the two conditions. Moreover, the authors themselves indicate that their machine learning classifier was unable to classify their home-cage data and as such, do not analyze the “control” group. Thus, without further statistical assessment, it is not appropriate to make general statements about the translational regulation induced upon “novel experience” (fear-conditioning) because there is no control group data analysis to compare it to.

      Low sequencing depth compromises reproducibility and leads to high replicate variability. In the analysis of deep-sequencing datasets, one maps the sequenced reads to a reference genome to identify the gene from which the transcript originated. With current RNA extraction, library preparation and sequencing techniques, the generally accepted lower-bound of “mappable” reads for an analyzable data set is around 75-80% (Sims et al.). In Ainsley et al. the average fraction of reads which yield useful information in all samples is low, (47.4%) leading to low sequencing depth; the analysis reported in Ainsley et al and our own re-analysis of the data agree on this (see our Figure 1A and B). Indeed, the fraction of mapped reads in the immunoprecipitated (IP) fraction (“ribosome-bound”) (which the authors focus their analysis on) is even lower than all other groups (< 40%) (our Figure 1A and B, http://brain.mpg.de/uploads/media/Ainsley_Rebuttal_01Sep2015.pdf). For comparison, a very similar recent study (using the same technique with a brain sample) showed a much higher fraction of mapped reads (Hupe et al., 2014). Although the authors report the use of a ribosomal RNA-depleted sample, (the Ovation RNA-Seq kit used for RNA amplification is not supposed to bind ribosomal RNA), a substantial fraction of their reads actually map to ribosomal RNA (Figure 1B). As a consequence, the genes detected in the sequencing replicates show very low gene overlap and the estimated RNA abundance is also poorly correlated (~ range 0.32 -0.72), again particularly in the IP fraction which is the focus of Ainsley et al.’s analysis (range 0.32-0.42) (our Figure 1C and D). For comparison, Hupe et al reported high replicability for their brain translatome data with all correlation values in excess of 0.98 (Hupe et al., 2014). Incorrect gene feature representation: Inclusion of non-coding RNA reads as mRNA reads. In the analysis of their data, Ainsley et al. map the sequencing reads to different domains of a gene e.g. reads aligned to the 5’UTR (untranslated region), coding sequence (CDS) and 3’UTR. In Figure 2a they report, surprisingly, that in different groups, between 22-80% of the reads map to the 3’UTR. Their annotation is in stark contrast to other published studies where, using similar techniques, an even distribution of reads throughout the gene body is typically observed (e.g. Hupe et al., 2014). In our Figure 2A (http://brain.mpg.de/uploads/media/Ainsley_Rebuttal_01Sep2015.pdf), using the raw published data, Ainsley et al.’s reads are independently mapped and the observed fractional annotation fails to confirm Ainsley’s report (our Figure 2A; compare to original Figure 2A in Ainsley et al). Indeed, the only way one can replicate their skewed (huge contribution of the 3’UTR reads) distribution is to include reads that map to non-coding RNA loci and erroneously assign them to the 3’UTR (our Figure 2B). The correct annotation of read position is important because Ainsley et al. go on to use these read positions in genes to train a classifier to identify mRNAs as pyramidal (+pyr) or non-pyramidal (-pyr).

      Flawed input, flawed design, and flawed output of a gene classifier. Ainsley et al used a training gene set to train a classifier to recognize transcripts as those transcripts arising from dendrites of pyramidal neurons (+pyr) or other cells in the neuropil (-pyr). The training set comprised 74 (+pyr) and 124 (-pyr) genes that the authors compiled by their own visual inspection of the Allen Brain Atlas. Unfortunately a significant fraction of these genes are completely absent from the author’s own analyzed dataset (40/74 +pyr genes and 38/123 -pyr genes missing, Supplementary Data 2 in Ainsley et al.). Furthermore, the authors propose, without any data to substantiate it, that reads from +pyr genes should be CDS-enriched and 3’UTR- de-enriched in their IP (“ribosome-bound”) fraction, relative to the supernatant fraction. Recreating the clustering procedure of Ainsley et al with adequate accuracy one observes that the genes are separated only by expression dominance in the IP fraction, independent of CDS or 3’UTR enrichment (Figure 2C). This graph reveals absolutely no clustering of genes, as would be expected if the author’s original formulation/idea were correct. Furthermore, we attempted to recreate the clustering using different pairs of biological replicates provided in the Ainsley et al study. The majority of replicates samples fail to successfully cluster the data with the same precision and accuracy as expected (clustering measures <0.5, Figure 2D). The above result is not surprising given the overall poor data quality, depth and expression correlation. This offers one explanation for why the authors were unable to classify their home-cage “control” dataset (Ainsley et al. page 4). In addition, we compiled a list of 139 in situ hybridization-verified dendritic mRNAs from several sources (Lein et al., Cajigas et al and references therein) and compared it to the “+pyr“ and “–pyr“ classified set suggested by Ainsley et al. (Figure 2E and 2F, Table 1 http://brain.mpg.de/uploads/media/Ainsley_Rebuttal_01Sep2015.pdf). We found that less than 35% of the dendritically-verified transcripts (from the above lists) were included in the Ainsley et al., (+pyr) list, the majority were in fact listed on the -pyr list. Even 16 genes that the Allen Brain Atlas team indicated as “dendritic” (e.g. Lein et al.,) were mis-classified by Ainsley et al. as (–pyr) (Table 1). In summary, the study of Ainsley et al., is flawed at many levels, including experimental design, poor data quality and incorrect analyses, invalidating many, if not all, of the conclusions of the authors.


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    1. On 2016 Apr 10, Lydia Maniatis commented:

      For the reasons described below, this introductory sentence has no content: "Noise can be used to characterize visual processing in noiseless conditions. For instance, contrast detection threshold in absence of noise is limited by both internal noise and the ability of detecting the signal embedded in noise, namely, calculation efficiency, which is inversely proportional to the smallest signal-to-(internal) noise ratio required to detect the signal."

      The stimulus consists of photons hitting the retina. Is this the "signal" according to these authors? No. The "signal" is a product of perceptual organisation to which the stimulus may give rise. This signal (e.g. a letter of the alphabet) has been designated a priori by the authors. If the stimulus is created by laying out a perceptible letter shape, and then adding dots overlying it, the additional dots will be called the "noise" even though they are a perfectly good "signal." The dots, called "external noise" will be supposed to represent "noise" and to constitute some kind of parallel to supposed "internal noise" that is supposed to mediate the percept (though to my knowledge no empirical tests of this assumption have been performed). The arbitrariness of the signal/noise dichotomy may be appreciated if we imagine that the letters themselves are composed of the same type of dots? Would we say the "signal" is composed of "noise?"

      What if, instead of dots, the "added noise" consisted of lines?

      Unless we specify that "noise" will always be defined as a specific structure, e.g. pixels of x visual angle and y luminance structure, then the effect of the arbitrarily defined "noise" on the arbitrarily designated "signal" will always depend on the physical characteristics of both and how they interact to influence the perceptual organisation of the stimulus. As has been demonstrated many times (e.g. by Gottschald, Kanizsa, Wertheimer), in some "noisy" conditions the "signal" may not be detectable at all, even if its contrast is high.

      Thus, referring to "noise" and "signal" in the abstract, without reference to structure, is meaningless. Therefore, the introductory sentence quoted above has no content.

      QED.


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    1. On 2014 Aug 06, Samir Ounzain commented:

      Thank you Dr Matkovich for clarifying these points, both myself and readers will appreciate this quick and comprehensive response. I understand that the review process can lead to absence of specific pieces of literature, especially those published in a comparable time frame. However typically in the process of revision it is important to cite even recently pubished work and discuss if highly relevant to your study. Many pieces of work are submitted months if not years before final acceptance but we all have a responsibility to correctly cite and discuss highly relevant recent work during any revisions. I would also like to clarify that citations 4 and 26 by the Hermann group and ourselves are not the most relevant in this context. Citation 24 is a review article and reference 4 describes Fendrr and not the recent more global characterisation of embryonic cardiac lncRNAs by the Herrmann group (for benefit of community these citations are in original post). For the benefit of everybody in this exciting new and emerging field it is of importance that all relevant and recent studies are included and discussed. Hopefully our discussion here as raised these points to the benefit of the field. I congratulate you on your important piece work, and especially your delineation of putative –cis control of proximal coding genes via lncRNAs characterised in your study. I think –cis control, especially for those lncRNAs templated by cardiac enhancers will emerge as an important regulatory function for the global enhancer reprogramming that underpins the re-activation of the fetal gene program and subsequent pathological remodelling. Your work provides further signficant evidence for the potential importance of lncRNAs in the developing and remodelling heart. I look forward to further studies from your Laboratory and the community. Functional and phenotypic characterisation of these exciting new cardiac enriched molecules is now of importance for all in the community.


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    2. On 2014 Aug 05, Scot Matkovich commented:

      I'm pleased that our recent publication has already attracted interested readers. With regard to the references we cited and the publication date of other literature in the field, we first submitted this paper to PNAS in November 2013; as is the trend at a lot of journals, the 'submission date' on the final paper is actually the receipt date of the most recent major revision (June 2014). We had already cited papers from the Herrmann and Pedrazzini groups as references 4 and 26. I would suggest that neither the peer review process nor the authors have been delinquent in failing to cite extremely recent literature, whose e-publication dates were largely coincident with the preparation of our revised manuscript.

      I would like to clarify one misrepresentation of our study made by Dr Ounzain. We did not attempt to identify 'novel' murine lncRNAs in the developing and adult heart, but rather sought to bring a degree of curation and refinement to the characterization of cardiac lncRNAs by focusing on a limited set of lncRNAs with strong evidence for existence as separate entities. We tried to avoid including database entries which may be spuriously annotated fragments of other RNAs, as indicated in our Supplemental Methods. Using this carefully selected set of lncRNAs, we evaluated the extent to which they were regulated during growth of the embryonic heart or pressure overload-induced hypertrophy. I feel it is likely that a similar disparity of lncRNA regulation between these two growth states will be found no matter how many lncRNAs are included in such a comparison.

      Nonetheless, I would like to thank Dr Ounzain for pointing out that his recent study provides a thorough catalog of 'known' and 'novel' murine cardiac lncRNAs as determined by ab initio reconstruction of paired-end RNAseq transcripts. As annotation improves with time and a common nomenclature for lncRNAs is decided, both of our raw sequencing read datasets should prove fruitful for others to mine and to investigate cardiac lncRNA regulation. The mechanistic studies we performed on reciprocally regulated lncRNAs and adjacent coding mRNAs should provide a useful framework for evaluating the extent to which other lncRNAs may regulate local transcription.


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    3. On 2014 Aug 04, Samir Ounzain commented:

      Overall a nice piece of work further extending the characterisation and identification of novel murine lncRNAs within the developing and adult heart post injury. However, sadly, a number of important publications predating the submission date of this manuscript were omitted.Specifically within introduction authors state ''Indeed, it is not yet known with certainty which lncRNAs are expressed in mouse hearts, nor have the identities of lncRNAs exhibiting 'cardiac-enriched' expression been defined''.

      These points have been addressed in previous publications and I kindly refer the authors of this manuscript and readers here on PubMed to the following important publications which were published prior to this paper being submitted. Sadly the peer review process also missed these

      1: Werber M, Wittler L, Timmermann B, Grote P, Herrmann BG. The tissue-specific transcriptomic landscape of the mid-gestational mouse embryo. Development. 2014 Jun;141(11):2325-30. doi: 10.1242/dev.105858. Epub 2014 May 6. PubMed PMID: 24803591.

      1: Ounzain S, Micheletti R, Beckmann T, Schroen B, Alexanian M, Pezzuto I, Crippa S, Nemir M, Sarre A, Johnson R, Dauvillier J, Burdet F, Ibberson M, Guigó R, Xenarios I, Heymans S, Pedrazzini T. Genome-wide profiling of the cardiac transcriptome after myocardial infarction identifies novel heart-specific long non-coding RNAs. Eur Heart J. 2014 Apr 30. [Epub ahead of print] PubMed PMID: 24786300.


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    1. On 2015 Jun 22, Eileen Daly commented:

      Dear Professor Bishop,

      Thank you so much for inviting us, through PubMed Commons, to reply to your comments on our Brain paper Response inhibition and serotonin in autism: a functional MRI study using acute tryptophan depletion. Your comments highlighted the differences between our paper and that of Chantiluke et al.’s 2015 paper Inverse fluoxetine effects on inhibitory brain activation in non-comorbid boys with ADHD and with ASD.

      From your comments, I sense your main issue is that our baseline data appears to differ from that of Chantiluke. This is of course a very interesting issue.

      There were many differences between the two studies that should be taken into account when comparing the findings.

      • The sample of Daly et al. was adults (mean age = 31) while that of Chantiluke et al. was pediatric (mean age = 15).

      • It is not correct that both studies used a Go/No-Go (GNG) task. The tasks were not the same. The study of Chantiluke compared successful stop with failed stop trials, whereas the study of Daly compared successful No-Go with oddball trials. While both studies controlled for the oddball effect, the task demands are different - the stop task is more challenging and has a lower load on selective attention than the GNG task.

      • The location of the right inferior frontal (R IFC) activation. The location of the R IFC underactivation in the study of Daly is in a more rostral and ventral location of ventrolateral prefrontal cortex at a z score between -12 and + 18 comprising BA 47, 10 and 46. It is hence a more ventral and rostral IFC region. In contrast the location of the IFC in the paper of Chantiluke only appears at + 30 to +40 and is in BA 44/9, - i.e. a far more dorsal and somewhat more caudal location. Therefore the two regions are not identical and the findings are consequently not inconsistent. Our most recent and yet unpublished (Lukito S, Carlisi C, Radua J, Simonoff E, Rubia K) meta-analysis of 13 inhibition fMRI datasets in 193 ASD children and adults shows in fact that the more dorsal location of IFC in BA 44/9 at a z-score of + 20 (comparable to IFC location in Chantiluke’s paper) is overactivated in ASD while a more ventral location in BA 47/46 at a z-score of 0 (comparable to the IFC location in Daly’s paper) is underactivated in ASD. The findings of the two papers are also in line with the findings of Kana et al., who found a more ventral location of IFC (BA 45) at + 10 to be underactivated in ASD, which corresponds to the IFC location of the study of our findings in Daly et al.

      • It is very difficult to compare the two baseline conditions across studies. First, Chanktiluke’s baseline is a true “placebo” condition, in that an “inactive’’ substance was utilized, as the placebo was peppermint water. In our study, however, the baseline condition is actually a “sham” procedure with a drink containing many “active” (i.e. crosses blood-brain barrier) substances, which were amino acids in our case. Thus, peppermint water has no physiological effect on brain functioning while our amino acid drink includes molecules that will exert a direct effect upon the baseline. This important issue may hence explain why differences in baseline conditions were reported.

      However, we would argue that the most consistent explanation for this apparent inconsistency and that is also in line with our recent meta-analysis of fMRI studies of inhibition in ASD is that there are two different IFC regions that are functionally abnormal in ASD during inhibition tasks. A more ventral and rostral region in BA 47/46 that is underactivated and a more ventral and caudal region in BA 44/9 that is overactivated. Serotonin modulation appears to normalize both deviant activations, in that it enhances the underactivated BA 47/46 cluster and it reduces the overactivated BA 44/9 cluster moving both activation patterns towards normality.

      Last, we wholehearted agree that the reproducibility in neuroscience and pharmacological intervention studies are critical. We also fully agree that this is an initial proof-of-concept study (albeit one that involved over 60 separate imaging experiments) that requires replication. However, our paper fully acknowledged this issue and used state-of-the art statistical approaches for analysing small samples (e.g. non-parametric statistics). Furthermore, we correct for multiple comparisons using standard methods (e.g. clusterwise for fMRI data and FDR for correlations). We were very pleased to observe that the finding of BA 46/47 underactivation was replicated in our meta-analysis in a much larger sample of 193 ASD patients and are hence confident in the finding.

      Again, we thank you for your invitation to reply to your comment and value your input.

      Sincerely,

      Dr Eileen Daly


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    2. On 2015 May 31, Dorothy V M Bishop commented:

      I was searching for the original source of a claim about autism by Declan Murphy: "we have found this brain abnormality, and we’ve been able to show we can reverse it" http://alumni.kcl.ac.uk/pioneers-appeal-professor-declan-murphy, and I came across this paper. I'm not sure if it the source of the claims: there is another paper on a closely similar topic with overlapping authors by Chantiluke et al (2015).

      I am puzzled, though, by the fact that these two papers seem to have inconsistent findings with regard to ASD, yet do not comment on this or cross-reference one another. Indeed, in the current paper, it is stated that: "to our knowledge, no one has investigated the modulatory effect of serotonin on inhibitory neural activity in individuals with ASD" (p 2601); the Chantiluke et al paper was not published at the time that Daly et al was submitted, but it was submitted two weeks later.

      Both papers look at behavioural and brain responses to a Go-NoGo task in individuals with ASD, with a child sample in Chantiluke et al, and adults in Daly et al. Serotonin levels are modified by fluoxetine administration in Chantiluke et al, and by tryptophan depletion in Daly et al. There are some procedural differences in the Go-NoGo task, but my impression is that these were not so great that one would expect to see a major effect on results. Yet quite apart from any impact of serotonin manipulations, the studies find different results in the placebo conditions. Daly et al find that "after sham, subjects with autism relative to control subjects, showed reduced activation in right inferior frontal cortex". In contrast, Chantiluke et al reported "Under placebo, relative to controls, ASD boys showed overactivation in left and right inferior frontal cortex (IFC)." (p. 2071).

      In the introduction to these papers, both cite prior work on inferior frontal cortex (IFC) and inhibition in autism. In particular, they make predictions based on another study by this group, by Schmitz et al, which also used fMRI to compare ASD and control groups during a Go-NoGo task. Schmitz et al reported significant increase in left middle/inferior (Brodmann area 10/46) and orbitofrontal gyrus during correct inhibition of NoGo trials, and no significant areas of decreased activation (p 11-12). Yet, Daly et al hypothesise that in the placebo conditions "subjects with ASD compared to controls would show decreased activation in right inferior frontal and increased activation in left inferior frontal cortices".

      The importance of reproducibility of research findings in neuroscience is receiving increased attention (Pernet & Poline, 2015), with growing recognition that there is a major problem for neuroimaging studies with small samples (Button et al., 2013), especially when, as in this case, multiway Anovas and correlations are computed without correction for multiple comparisons. Pharmacological interventions that 'normalise' brain abnormalities are potentially of huge interest, but they are unlikely to reflect more than error of measurement and regression to the mean if baseline differences are not reproducible.

      It may be that there is some simple explanation for these inconsistencies; it would be good to hear the authors' views on this.

      References Button, K. S., Ioannidis, J. P. A., Mokrysz, C., Nosek, B. A., Flint, J., Robinson, E. S. J., & Munafo, M. R. (2013). Power failure: why small sample size undermines the reliability of neuroscience. Nature Reviews Neuroscience, 14, 365-376. doi: 10.1038/nrn3475

      Chantiluke, K., Barrett, N., Giampietro, V., Santosh, P., Brammer, M., Simmons, A., Murphy, D., & Rubia, K. (2015). Inverse fluoxetine effects on inhibitory brain activation in non-comorbid boys with ADHD and with ASD. Psychopharmacology, 232(12), 2071-2082.

      Pernet, C., & Poline, J.-B. (2015). Improving functional magnetic resonance imaging reproducibility. GigaScience, 4(15). doi: 10.1186/s13742-015-0055-8

      Schmitz, N., Rubia, K., Daly, E., Smith, A., Williams, S., & Murphy, D. G. M. (2006). Neural Correlates of Executive Function in Autistic Spectrum Disorders. Biological Psychiatry, 59(1), 7-16


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    1. On 2014 Aug 13, Amanda Capes-Davis commented:

      Zhao et al published a paper in 2011 (PMID 21868764) to show that ARO is not an appropriate model for anaplastic thyroid carcinoma. ARO is a misidentified cell line, meaning that it does not come from the original donor. ARO is actually HT-29, a colon carcinoma cell line. For a list of known misidentified cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2014 Oct 08, David Keller commented:

      Screening the Pap smear plus HPV status in parallel improves overall sensitivity

      Dr. Feldman's recommendation to continue screening with the Pap test makes sense; the Pap smear directly detects malignancy and worrisome pre-cancerous cellular changes. High-risk HPV is an infection which can cause cervical cancer, but testing for HPV does not provide direct evidence of the presence or absence of cervical cancer and its precursor lesions. Women die of cervical cancer, they do not die from HPV infection. The HPV test and the Pap test provide complementary information, there is unique information learned from each test when they are both performed, and screening sensitivity is enhanced when 2 such tests are performed in parallel (1). Screening women for cervical cancer without any examination of cervical cytology does not seem prudent at this time.

      Reference

      1: Fletcher RH, Fletcher SW. Clinical Epidemiology: The Essentials Lippincott Williams & Wilkins, 2005: 4th ed


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    1. On 2014 Nov 06, Hugues Lefort commented:

      I would ligke to know if it is possible to modify the last name of an autor in a publication such this one. The first author is "Lefort H". It's seem that Elsevier has send three times an email to pubmed, so did I... and no modification yet. Thank you for your lights.


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    1. On 2014 Nov 24, Guillaume Filion commented:

      This article is one of the "CISCOM meta-analyses", which are very similar papers written by different authors. For more information about the CISCOM meta-analyses, check the blog post "A flurry of copycast on PubMed" at the following link http://blog.thegrandlocus.com/2014/10/a-flurry-of-copycats-on-pubmed


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    1. On 2014 Nov 17, Raphael Levy commented:

      Comments by Philip Moriarty (Nottingham, UK) and Quanmin Guo (Birmingham, UK) are available at PubPeer. They raise questions on the interpretation of the images shown by Ong et al.

      The article belongs to the “stripy nanoparticles” series. The evidence behind the structure and special properties of these nanoparticles has been challenged by Cesbron Y, 2012. The publication in 2012 of Cesbron Y, 2012 took three years and has been followed by post-publication peer review of the various existing and new stripy articles on my blog, PubPeer, etc.

      A detailed analysis of the evidence for stripy nanoparticle is published today in PloS One by Stirling et al; from the abstract: “through a combination of an exhaustive re-analysis of the original data with new experimental measurements of a simple control sample comprising entirely unfunctionalised particles, we conclusively show that all of the STM evidence for striped nanoparticles published to date can instead be explained by a combination of well-known instrumental artefacts, strong observer bias, and/or improper data acquisition/analysis protocols.


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    1. On 2014 Aug 09, Seyed Moayed Alavian commented:

      Occult HCV infection is a new entity and we need to more studies for better clarification the issue

      Hepatitis C is an important etiology for chronic liver disease and it is the most common cause in chronic renal failure patients. Recently, occult HCV infection has described with the absence of HCV-RNA and anti-HCV antibodies in serum in the presence of genomic HCV-RNA in the liver biopsy specimen, in patients who suffer from cryptogenic liver diseases. Furthermore, about 70% of patients with occult HCV infection also have HCVRNA in their peripheral blood mononuclear cells (PBMCs); the genomic and the antigenomic HCVRNA have also been detected in these cells. The detection of antigenomic HCV-RNA strand in PBMCs of subjects with occult HCV infection can be supported the hypothesis that HCV is able to replicate in these cells. Patients on hemodialysis are at higher risk for HCV infection and HCV infection has a bad impact on survival of patients after renal transplantation. The anti-HCV antibody can be negative in these patients and in sometimes we have some cases that are negative for HCV infection before renal transplantation and after it, the HCV infection appears and may be some cases had occult HCV infection and after using the immunosuppressive drugs HCV will appear. I suggest to be more sensitive regarding the occult HCV infection in hemodialysis patients. Ref: Bokharaei-Salim F, Keyvani H, Monavari SH, Alavian SM, Madjd Z, Toosi MN, et al. Occult hepatitis C virus infection in Iranian patients with cryptogenic liver disease. J Med Virol. 2011;83(6):989-95


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    1. On 2014 Aug 05, Sergio Uribe commented:

      For anyone interested, here is the 1st clinical report about approximal therapeutic sealants (in spanish): http://j.mp/1QwmeAd


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    1. On 2014 Aug 12, Karim Asehnoune commented:

      In the CRASH trial, mild to severe TBI patients (GCS<14) were included, and a short course of high-dose methlyprednisolone was used. In the CORTI-TC study, only severe TBI patients (GCS<8 and abnormalities on brain CT-scan) were included, and low dose of steroids (hydrocortisone)+fludrocortisone were used. When comparing these 2 studies, one could say: the population is different, the drugs used are different, the outcomes are different. One book is closed, the other one remains open.


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    2. On 2014 Aug 10, Ryan Radecki commented:

      Post-publication commentary:

      "A Moratorium on Steroids for TBI"

      In 2004 the CRASH trial examining the efficacy of steroids for acute traumatic brain injury (TBI) was published in The Lancet. This massive trial included over 10,000 patients was stopped prematurely because of an increased mortality in the patients who received corticosteroids. This should have definitively closed the book on such a therapy. Despite this damning evidence, it appears all one has to do to make this question relevant again is to devise a disease-oriented endpoint with plausible clinical relevance and test it using a sample size too small to differentiate these harms from the surrounding noise of statistical chance.

      http://www.emlitofnote.com/2014/08/a-moratorium-on-steroids-for-tbi.html


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    1. On 2015 Dec 11, Deborah Ritter commented:

      It is ZNF444, not ZNF44. Throughout the article, they use ZNF444 and the referenced article uses ZNF444. I contacted to publisher to report the mistake and was told they cannot change it.

      Dear Dr Ritter,

      Thank you for your email.

      We can no longer correct the article because it is already published in an issue.

      Regards,

      Production Editor On behalf of Wiley Manila

      From: cs-author@wiley.com Sent: Thursday, December 03, 2015 10:33 AM To: Subject: URGENT --- correct ZNF44 in abstract to ZNF444 Your case 00636351 [ ref:00Dd0eeku.500d0f4DMy:ref ]

      Dear Deb,

      Histopathology - Vol 65, Iss 6, Dec 2014 "Myoepithelioma of bone with a novel FUS-POU5F1 fusion gene" DOI: 10.1111/his.12517

      Thank you for your recent communication regarding a correction to the above article.

      We understand your concern, hence, we have copied the journal's Production Editor into this email, as they are in the best position to assist you further. They will be contacting you shortly. Your patience in the meantime is much appreciated.

      Arjane, we would greatly appreciate if you could please assist with the customer's inquiry regarding a typographical error as detailed in their email below. They are asking if this can possibly be corrected. Please respond to the customer directly at dritter@bcm.edu.

      Kind regards,

      Wiley Author Support

      If you require further assistance with this matter or would like information on any of our other journals please visit Online Get Help to assist with many of your queries 24 hours a day, 7 days a week.

      --------------- Original Message --------------- From: Sent: 12/2/2015 8:40 AM To: cs-journals@wiley.com Subject: correct ZNF44 in abstract to ZNF444 {500d000000f4DMyAAM.003d000002imvxXAAQ}

      Hi,

      I recently found an article from Genes Chromosomes Cancer on myoepithelioma of bone, and I was interested in ZNF44 gene, which is mentioned in the abstract. However, throughout the rest of the article (and in the referenced article about fusion with EWSR1) the gene is ZNF444. It looks like there is a typo in the abstract for ZNF44 instead of ZNF444, and I just wanted to send a quick note about it to be corrected if possible.

      http://www.ncbi.nlm.nih.gov/pubmed/25066216

      Thank you,

      Deb


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    1. On 2016 Jun 24, Lily Chu commented:

      The limitation with this study is that symptoms were only recorded within a 24-hour period. Many patients with ME/CFS suffer from post-exertional malaise. Post-exertional malaise can start after 24 hours have passed and can endure for longer than 24-hours. Patients are often able to perform activities once or for a short period but the difficulty is when they have to repeat it again the same day or over the next few days. Repeated cardiopulmonary testing shows drops in cardiometabolic parameters not during a first exercise test but during a repeated test the next day. One study, for example,

      https://translational-medicine.biomedcentral.com/articles/10.1186/1479-5876-12-20

      http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4004422/

      Similarly, see this study which follows symptoms for more than 24 hours.

      http://www.ncbi.nlm.nih.gov/pubmed/20095909

      Finally, clinicians should be careful about prescribing aerobic exercise. On average about 50% of patients report worsening of their health if exercise is prescribed without careful consideration of symptoms that flare up. http://www.ncf-net.org/library/Reporting of Harms.pdf


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    1. On 2016 Dec 30, Arturo Martí-Carvajal commented:

      I would like to ask the following: How should figure 4 be understood? That funnel plot only has 6 trials.


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    1. On 2014 Oct 14, Anders von Heijne commented:

      The authors quite correctly identify that making prior imaging available to the current institution and formally summarizing their findings as one of the greatest opportunity to provide value to the health care system in order to avoid unnecessary repeat examinations. When patients are transferred between providers the referring physician commonly summarizes the case and its course in discharge notes. In radiology, however, the chore of collecting and compiling the performed radiology is usually done at the receiving hospital. It stands to reason that if the equivalent of radiological discharge notes instead are created at the department performing the examinations, the quality of the summaries must be improved, as well as the content of the transferred information, to the benefit of both clinicians and radiologists at the receiving hospital.


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    1. On 2014 Aug 10, Ryan Radecki commented:

      Post-publication commentary:

      "Get to the Choppa! Or ... Maybe Not?"

      Helicopter transport is entrenched in our systematic management of trauma. It is glamorized on television, and retrospective National Trauma Data Bank studies seem to suggest survival improvement – and those with head injury seem to benefit most.

      But, these NTDB studies encompass heterogenous populations and are challenged in creating truly equivalent control groups. This study, on the other hand, is a single-center experience, allowing greater consistency across divided cohorts. In a novel approach, these authors collected all HEMS trauma transfer requests to their facility across their 30-county catchement area – and specifically looked at occasions when weather precluded HEMS. This therefore created two cohorts of patients eligible for HEMS, with a subset that was transported by ALS due to chance events. The paramedic crews manning the HEMS and ALS transfers were staffed by the same company, and therefore had roughly equivalent training....

      http://www.emlitofnote.com/2014/08/get-to-choppa-or-maybe-not.html


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    1. On 2015 Aug 17, Phyllis Mervine commented:

      Why does PubMed include this 2004 review at the top of the list among studies published in 2014-15?


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    1. On 2015 Aug 17, Phyllis Mervine commented:

      Why does PubMed include this 2003 review at the top of the list among studies published in 2014-15?


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    1. On 2015 Aug 07, Serge R Mordon commented:

      Dr Liu and the co-authors of this article must be congratulated for this very interesting and important clinical study.


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    1. On 2014 Jul 30, Jim Woodgett commented:

      The GSK-3beta inhibitor used here, SB216763, is equipotent towards GSK-3alpha, a highly related isoform that plays equivalent roles to GSK-3beta in regulation of Wnt (and other) responses.


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    1. On 2015 Jun 18, Elsamma Chacko commented:

      This is about very intense pre-meal exercise is not good for glucose control; There can be post exertion glucose elevation.


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    1. On 2014 Jul 25, Ryan Radecki commented:

      Post-publication commentary:

      "The Scandal of Dabigatran – A Summary"

      We’ve been desperate for a more elegant solution to anticoagulation than rat poison for seemingly an eternity. Now, we have them: direct thrombin and factor Xa inhibitors. The studies supporting their use seem favorable.

      But, as the old story goes – and as previously reported on this blog many times – Boehringer Ingelheim has been selectively reporting only the most favorable aspects of their flagship drug, dabigatran. Increased cardiovascular events have been downplayed through study design not powered to detect a difference. Issues with fixed dose therapy – and lack of a range of options for patients with renal impairment – rear their ugly head in multiple case reports....

      http://www.emlitofnote.com/2014/07/the-scandal-of-dabigatran-summary.html


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    1. On 2014 Oct 04, Quentin Hill commented:

      In the section on guidelines, the authors have stated that the current British Committee for Standards in Haematology guidelines Davies JM, 2011 recommend lifelong penicillin prophylaxis for all persons with surgical asplenia. Although this was true in previous guidelines Working Party of the British Committee for Standards in Haematology Clinical Haematology Task Force., 1996, Davies et al recommend a risk adapted approach to antibiotic prophylaxis. They recommend antibiotic prophylaxis "at least" in the immediate post-operative period following splenectomy for trauma. Otherwise, long term prophylaxis is recommended for those considered to be high risk of pneumococcal infection: age <16 years or >50 years, inadequate serological response to pneumococcal vaccination, previous invasive pneumococcal disease and splenectomy for underlying haematological malignancy.

      Additionally, the authors do not discuss the meningitis serogroup B vaccine (MenB). A MenB vaccine was licensed by the European Medicines Agency in January 2013. Although not yet FDA licensed, it has been used to control several outbreaks in the United States http://www.cdc.gov/meningococcal/outbreaks/vaccine-serogroupb.html. In England, over 80% of Neisseria meningitidis cases are due to capsular group B strains and it has been recommended in England for children and adults with asplenia, splenic dysfunction and complement disorders https://www.gov.uk/government/collections/immunisation-against-infectious-disease-the-green-book.


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    1. On 2014 Jul 31, Amanda Capes-Davis commented:

      Please be aware when choosing cell line models that some are misidentified and do not correspond to the expected tissue or disease. The KB cell line is one example of a misidentified cell line. It is cross-contaminated with HeLa and is actually cervical adenocarcinoma, not oral squamous cell carcinoma. For a list of known misidentified cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2015 Apr 14, RheumJC - Rheumatology Twitter-Based Journal Club commented:

      This article was discussed on March 3rd, 2015 by participants of #RheumJC, an international Twitter-based Rheumatology Journal Club. An engaging discussion on the science of the topic as well as the methodology of the study was had over 2 different one hour live "chats" as well as a full 24hr of asynchronous participation. Included in the second live session was the participation of the study lead author, Dr. Miloslavsky (@emilosla). Overall (combined sessions and time between and after) there were 46 total participants from 17 different countries. For the full 24 hours, there were 518 total tweets – 387 unique tweets and 117 RTs

      A slide-show summary of the sessions was compiled by Lois Wingerson (@RheumatologyNet) and can be seen at http://www.rheumatologynetwork.com/vasculitis/rheumatology-journal-club-2-rituximab-aav-relapse

      We would like to thank Wiley and A&R for making this manuscript open access leading up to this journal club.

      Interested individuals can track and join in future journal clubs by following @RheumJC or #RheumJC, or visit the webpage at http://www.rheumjc.com and sign up for announcements.


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    1. On 2016 Mar 04, Andrea Margulis commented:

      Diabetes progression and the consequent need for intensification of treatment occur in stages over time, with feedback loops and several influences including those from diabetes complications, comorbid conditions, and concomitant medications. The resulting web of prognosis, prescription, and disease progression over time creates methodological challenges for research on the effect of diabetes treatments [1,2]. Patients under different diabetes therapies may have very different baseline characteristics that may be only partially amenable to standard observational research techniques for confounding control. As patients pass through different stages of diabetes, treatment escalates or changes, and these updated therapeutic schemes may become indicators for a more severe stage of diabetes with a more guarded prognosis. In addition, each medication carries its own risks. In this situation, it becomes unclear how to validly assess exposure to earlier medications such as metformin, since continuing follow-up under a new therapeutic scheme mixes exposure effects and disease progression together, while stopping follow-up to isolate exposure to earlier therapeutics may create a bias similar to the differential loss to follow-up than can affect randomised controlled trials (informative censoring).

      Challenges increase in the context of a comparison between treated diabetic patients and non-diabetic patients, as Bannister and colleagues [3] did with regard to the assessment of all-cause mortality. The authors report a 15% survival benefit in patients with diabetes on metformin monotherapy relative to patients without diabetes who were not on metformin, even though patients with diabetes were sicker at baseline. Results were consistent across subgroups, and a similar benefit was not observed for sulfonylurea treatment. This study addresses an important question, as previous research on metformin has produced promising findings, such as the ability to prolong lifespan and improve healthful aging in mice [4].

      Although the results from Bannister et al. [3] are intriguing, we wonder whether study design features might have created a cohort of patients with diabetes that selectively retained healthier individuals, while the same was not true for the cohort without diabetes to which they were compared. To identify the effect of metformin or sulfonylurea monotherapy, follow-up of treated patients with diabetes was censored after any modification to the initial treatment. Thus, as patients with diabetes progressed to the point they needed treatment intensification, they left the cohort. In contrast, the patients without diabetes would not have the chance to be excluded from the cohort in a similar manner with any progression from a starting point of good health. This censoring is tied to the mortality outcome since if a patient with diabetes dies, the matched comparator patient cannot leave the cohort until he or she dies. On the other hand, if the comparator without diabetes dies first, the matched patient with diabetes can still leave the cohort upon treatment modification. This creates a different opportunity for mortality to be observed in the two cohorts.

      Furthermore, the requirement of patients with diabetes to stay on glucose-lowering therapy for 180 days to be eligible (while comparators without diabetes are only required to survive for the 180 days) may have created an additional opportunity to selectively retain healthier individuals, i.e., adherent patients. Good adherence by itself has been shown to reduce mortality [5]. In subgroup analyses where patients with and without diabetes received cardiovascular prophylaxis (making them more similar in terms of adherence) the survival benefit decreases or disappears.

      While the authors have posed an interesting and relevant research question, it is accompanied by many difficulties from a methodological perspective. It may be worth considering an alternative comparison cohort comprised of non-diabetic persons with treatment for some other chronic condition, for which an analogous run-in period and censoring upon treatment intensification could be applied. Such an approach would enhance comparability of the cohorts at baseline and provide similar opportunity for follow-up to stop when patients in either cohort change treatment; all of which would mitigate the healthy adherer effect in the comparison group. The validity of this approach would depend on the possibility for both arms to follow similar patterns of treatment modification in relation to the risk of death. This proposed alternative approach has the drawback of answering a somewhat different research question, but one that may be more amenable to observational investigation.

      Andrea V Margulis, MD, ScD <sup>1</sup>

      Manel Pladevall, MD, PhD <sup>1</sup>

      Nuria Riera-Guardia, PhD <sup>1</sup>

      John Seeger, PharmD, DrPH <sup>2</sup> <sup>3</sup>

      Elisabetta Patorno MD, DrPH <sup>2</sup>

      Cristina Varas-Lorenzo, MD, PhD <sup>1</sup>

      <sup>1</sup> RTI Health Solutions

      <sup>2</sup> Division of Pharmacoepidemiology and Pharmacoeconomics, Department of Medicine, Brigham & Women’s Hospital/Harvard Medical School

      <sup>3</sup> Optum Epidemiology

      REFERENCES

      1 Patorno E, Patrick AR, Garry EM, et al. Observational studies of the association between glucose-lowering medications and cardiovascular outcomes: addressing methodological limitations. Diabetologia. 2014 Nov;57(11):2237-50.

      2 Suissa S, Azoulay L. Metformin and the risk of cancer: time-related biases in observational studies. Diabetes Care. 2012 Dec;35(12):2665-73.

      3 Bannister CA, Holden SE, Jenkins-Jones S, et al. Can people with type 2 diabetes live longer than those without? A comparison of mortality in people initiated with metformin or sulphonylurea monotherapy and matched, non-diabetic controls. Diabetes Obes Metab. 2014 Nov;16(11):1165-73.

      4 Martin-Montalvo A, Mercken EM, Mitchell SJ, et al. Metformin improves healthspan and lifespan in mice. Nat Commun. 2013;4:2192.

      5 Granger BB, Swedberg K, Ekman I, et al. Adherence to candesartan and placebo and outcomes in chronic heart failure in the CHARM programme: double-blind, randomised, controlled clinical trial. Lancet. 2005 Dec 10;366(9502):2005-11.


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    1. On 2014 Aug 16, M P M Hensgens commented:

      Dear Peter English, It is indeed correct that we did not study the cost effectiveness of increased testing for C. difficile. In this manuscript we showed that C. difficile occurs in a fair amount in general practitioners practice, although many still consider the disease as nosocomial. Now that we know that the bacterium occurs in this setting, a study concerning the cost effectiveness is an aim for future reseach. Thank you for your interest and kind regards, Marjolein Hensgens


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    2. On 2014 Aug 15, Peter English commented:

      I didn't spot anything about the costs and benefits of dramatically increasing the amount of testing that this paper is recommending.

      If you do a lot more tests for C diff infection, the costs to laboratories and health systems of doing the tests and acting on the results will be considerable. Most health systems have limited resources: money spent on this will have to be taken from something else. That might be worth while; but to be sure, we have to know if the value of doing this (in terms of e.g. reduced years of life lost, QALYs, reduced costs of treatment, reduced sickness/carers' absenteeism and resulting lost revenues etc.) are sufficient to justify the additional costs.

      Perhaps I missed this in the paper; but I don't think this was done.


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    1. On 2014 Jul 24, Ryan Radecki commented:

      "You Can Use Absorbable Sutures Anywhere"

      Although, can and should are entirely different interpretations of these data.

      There have been many studies showing facial lacerations can be repaired with absorbable sutures with similar cosmetic and adverse outcomes compared with non-absorable sutures. The same principles, presumably, hold for the trunk and extremities – although, there are significant differences in blood supply and healing time....

      http://www.emlitofnote.com/2014/07/you-can-use-absorbable-sutures-anywhere.html


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    1. On 2015 Jun 04, Christina Niederstadt commented:

      The authors tell us their “data on overall survival appeared interesting” - especially concerning "Overall survival from date of diagnosis of metastatic disease". They fail, however, to say anything about possible influences of "later Treatment for Metastases" on overall survival.<br> The only two patients who were, apparently, still alive at the end of the trial did receive either two times surgery (patient I-C14) or treatment with a protein kinase C inhibitor (patient VIII-A4).

      The sustained survival of those two patients could well be attributable to the method of "later Treatment for Metastases" - as might be the case with part or all of the other patients, too.


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    1. On 2014 Aug 05, Peter English commented:

      Given the apparent success of vaccination of pregnant women at 29+ weeks gestation, is there any point in trying to achieve something as difficult as coccooning? It's next to impossible to do, systematically. Is there evidence that it is significantly more effective than vaccination of pregnant women?


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    1. On 2017 Mar 16, KEVIN BLACK commented:

      This report gives some useful information but I interpret the results quite differently. The authors start with the assumption that the trough level is what one wants. I disagree. What one wants is to be able to compare a patient's lithium dosing to the large body of published knowledge about lithium treatment. Almost all of that data comes from standard 12-hour blood draws with plain (immediate-release) lithium carbonate or citrate. So the real question of interest is, with extended-release lithium formulations, at what time point do I draw the lithium level to compare most accurately with a standard 12-hour blood draw with plain lithium carbonate? The answer is not obvious because extended-release formulations affect only the absorption and not the excretion of lithium. Their primary benefit is reducing the transient peak lithium serum concentration, not delaying the (already relatively slow) elimination of lithium.

      Emami J, 2004 provide the needed data. They show, first, that 90% of the administered dose of a commercial extended-release formulation (Eskalith CR®) is absorbed by 4 hours after a dose, and ~100% is absorbed by 8 hours (Fig. 2A). Second, they show that at 12 hours after a dose, the blood levels for immediate and extended release formulations are essentially identical (Fig. 3). Thus 12 hours after the last dose is the ideal time for drawing blood levels for extended-release lithium tablets.


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    1. On 2014 Sep 23, Samir Ounzain commented:

      The potential for lncRNAs to serve as biomarkers in cardiovascular disease is very exciting and warrants further investigation. In an editorial associated with this interesting study from Vausort et al, Skroblin and Mayr raise a couple of very interesting points that need further investigation and discussion.

      They state ''All selected lncRNAs have been identified in noncardiac tissues. This lack of cardiac specificity questions their usefulness as predictors of cardiac dysfunction. At best, measuring lncRNA expression in full blood might reflect inflammation at the site of MI''.

      We agree strongly with this statement and would like to emphasise that cardiac specific/restricted lncRNAs likely represent the most important candidates both as biomarkers but also as highly specific therapeutic targets for future manipulation. Indeed, we recently demonstrated that through utilising very deep RNA-sequencing coupled with ab initio transcript reconstructions it is possible to identify 1000s of novel heart specific lncRNAs. Importantly we feel sequencing to a high depth, in a very specific context (we sequenced to a depth of 400x106 PE-reads per sample in isolated border zones post myocardial infarction, as compared to 50x106 PE-reads used in most comparable studies)is critical for the idenfication of highly cell/tissue and context specific lncRNAs, that ultimately we believe will represent the most attractive biomarkers and therapeutic targets.

      It is worth noting that when utilising this approach, we found that novel previously unknown lncRNAs were both a) much more cardiac specific than mRNAs and annotated lncRNAs (indeed many exhibit cell type specificity within the heart, b) were better correlated with cardiac physiological traits vs cannonical biomarker mRNAs and annotated lncRNAs, supporting the notion novel heart enriched lncRNAs could represent very attractive biomarkers, c) were highly associated with unique heart specific chromatin signatures linked to active -cis control enhancers, again has implications in therapeutic settings as enhancer reprogramming post stress underpins the fetal activation of gene program that is implicated in pathological remodelling and finally d) using a novel approach to infer lncRNA functions based on developmental chromatin state transitions, we found that novel lncRNAs were highly enriched in functional clusters linked to very specific cardiac functional processes including contractility etc.

      Many of the novel lncRNAs we identified in this study were conserved in human, and we hope future studies will leverage our data for the identificaiton of novel heart specific biomarkers that may be circulating in the blood. The excellent cohort described here and assesed by the Devaux group could represent a great starting point to asses these heart specific lncRNAs. Most studies to date have only assesed the annotated long non-coding transcriptome in this setting, and we believe our paper demonstrates that novel cardiac enriched lncRNAs are likely much more interesting candidates for analysis.

      For those interesting in these novel heart specific lncRNAs, and their potential utility as a biomarker, please refer to..

      Ounzain S, Micheletti R, Beckmann T, Schroen B, Alexanian M, Pezzuto I, Crippa S, Nemir M, Sarre A, Johnson R, Dauvillier J, Burdet F, Ibberson M, Guigó R, Xenarios I, Heymans S, Pedrazzini T. Genome-wide profiling of the cardiac transcriptome after myocardial infarction identifies novel heart-specific long non-coding RNAs. Eur Heart J. 2014 Apr 30. [Epub ahead of print] PubMed PMID: 24786300.


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    1. On 2015 Apr 29, Andrew Brown commented:

      Our letter discussing concerns about the conclusions of this article can be found here Bohan Brown MM, 2015, and the authors' responses here Kiecolt-Glaser JK, 2015.


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    1. On 2014 Sep 27, David Keller commented:

      Pembrolizumab first-line for metastatic melanoma & preexisting autoimmune disease?

      Patients with preexisting autoimmune diseases were excluded from the landmark trials of ipilimumab and pembrolizumab, which therefore cannot provide high-quality safety data for these patients. The grade 4 (life-threatening) and grade 5 (fatal) adverse events for both medications were primarily autoimmune in nature, in trial patients with no history of autoimmune disease. Pembrolizumab appears to have a somewhat lower rate of severe-to-fatal adverse events than ipilimumab, although no head-to-head comparison is available.

      Pembrolizumab was recently approved by the FDA for treating metastatic melanoma patients who have disease progression following ipilimumab. Medicare and private insurers are quite strict about not paying for off-label use of pembrolizumab, even for patients with active autoimmune disease. I have personally corresponded with two authors of this paper who advocate first-line treatment using pembrolizumab in selected clinical scenarios, for enhanced patient safety. Although there is controversy on this question in the immuno-oncology community, it seems reasonable to let treating oncologists decide when pembrolizumab should be used first-line and off-label for selected high-risk patients, pending their inclusion in randomized trials. As matters now stand, the wealthy who can pay cash for pembrolizumab effectively have access to a treatment option not available to less-wealthy melanoma patients. The FDA should reconsider their narrow prescribing indication for pembrolizumab, the adverse effects this may have on melanoma patients with preexisting autoimmune diseases, and the disparity caused by expensive off-label treatment options which are available only to patients who can pay the very large cash price in advance.


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    1. On 2014 Dec 18, CREBP Journal Club commented:

      The new plain language summary (PLS) evaluated was substantially revised from the current one in the Cochrane systematic review, although it maintained the narrative format. We would have preferred a three-arm RCT (new PLS format vs. revised current PLS vs. current PLS). The group discussed what proportion of correct responses is realistic for the public (or indeed health professionals) to attain? Also, how might people or health professionals be taught to assist their understanding of this format? More respondents exposed to the new PLS format strongly disagreed with the statement “The information is reliable" (Figure 4, pg. 8) and poses the question whether improving understanding of the quality of evidence paradoxically introduces a level of uncertainty. We also wondered whether the wording of questions may have introduced bias – for example, the question on the comprehension of the purpose of the summary (ie. “This summary is about the results of a large study”; Yes/No/I’m not sure) might be correctly interpreted as a single study or a systematic review and meta-analysis. The evaluation of ‘creative language’ used in standardised qualitative statements about treatment effects might also introduce bias. Despite carefully defining standardised qualitative statements in relation to distinct levels of evidence (eg. ‘will’=high level of evidence; ‘probably’=moderate level of evidence) they were combined on one occasion which was counter-intuitive (eg. “Probably will not decrease how long a cold lasts…”). See CREBP Journal Club Page for more


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    1. On 2014 Dec 10, Kath Wright commented:

      Other search filters are available from the InterTASC Information Specialists' Sub-Group Search Filter Resource at https://sites.google.com/a/york.ac.uk/issg-search-filters-resource/home


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    1. On 2014 Jul 30, Jung Weon Lee commented:

      The coauthor Kim S should be affiliated with "5 Therapeutic Antibody Research Center, Korea Research Institute of Bioscience and Biotechnology, Daejon, Republic of Korea", rather than "Department of Biological Sciences, Kangwon National University".


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    2. On 2014 Jul 31, Amanda Capes-Davis commented:

      Thank you for your reply. Yes, it is important to use a range of cell line models. It is also important to spread the word that Chang cells are not an appropriate model for liver. Authentication testing using a method such as short tandem repeat (STR) profiling will help to confirm that cell lines used in experimental work are not misidentified.


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    3. On 2014 Jul 30, Jung Weon Lee commented:

      In this study, many different liver cells in addition to HCC827 (NSCLC) and Chang cells were used in parallel.


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    4. On 2014 Jul 29, Amanda Capes-Davis commented:

      Although they carry the name "Chang liver", these cells are not from normal liver. The Chang liver cell line is cross-contaminated with HeLa and is actually cervical adenocarcinoma. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2014 Jul 20, Annie De Groot MD commented:

      By the way there is already concern that H7N9 is immmune-modulating on its own. Would immune-modulating drugs help, or hinder protection against severe disease?


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    1. On 2014 Jul 21, Thomas Crouzier commented:

      Very interesting to learn that lubricin has such an effect.

      In a recent study (Crouzier T, 2013), we also showed that mucins can effectively prevent the adhesion of mammalian cells. The effect was dependent on mucins and mucin source as well as the surface chemistry.


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    1. On 2014 Sep 06, Ryan Radecki commented:

      Post-publication commentary:

      "Still Adrift in Ignorance Over Blood Cultures"

      While supervising residents, one of the frequent diagnostic suggestions in undifferentiated febrile patients is: blood cultures. As an Emergency Physician, the utility of blood cultures – short of diagnosing endocarditis or another primary hematogenous source – is vanishingly small. After all, the source of infection is nearly universally somewhere else – lung, urine, CSF, skin & soft tissue – and relying on the blood to give you the answer two days later is an unreliable and impractical proposition.

      This study is yet another attempt at identifying patients with high likelihood of bacteremia, retrospectively analyzing 5,499 patients at Odense University Hospital for whom blood cultures were drawn....

      http://www.emlitofnote.com/2014/09/still-adrift-in-ignorance-over-blood.html


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    1. On 2014 Nov 18, Helen E Benson commented:

      Ligands and proteins specified in this paper are linked to the corresponding IUPHAR/BPS Guide to Pharmacology database entries via this blog post.


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    1. On 2014 Jul 29, Amanda Capes-Davis commented:

      Please be aware that "Chang liver" cells are actually not from liver. The Chang liver cell line is known to be cross-contaminated with HeLa and comes from cervical adenocarcinoma. For a list of known cross-contaminated cell lines, see http://iclac.org/databases/cross-contaminations/.


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    1. On 2014 Oct 29, Roman Stilling commented:

      Thank you for the comment. We realized that the paper is not associated with the search term "Gcn5" in Pubmed, hence I posted this comment. I had hoped that if the term appears in the comments it would appear in the search results, but it doesn't, as you pointed out correctly. While personally I'm all for "rationalizing" gene names, since today most genes are associated with a lot more functions than the name would suggest, I think databases should be able to deal with synonyms, i.e. Pubmed should show results for Gcn5 when Kat2a was searched and vice versa. It works well in the NCBI Gene database, so why not in Pubmed?


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    2. On 2014 Oct 22, L Charles Murtaugh commented:

      A good example of the unintended consequences of "rationalizing" gene names - rendering opaque almost 30 years of literature! Note that if one searches Pubmed for "Gcn5," this paper does not appear among the hits.


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    3. On 2014 Oct 18, Roman Stilling commented:

      For clarification of this abstract, it may be worth noting that K-Lysine acetyltransferase 2a (Kat2a) is more widely known by its former name General control of amino-acid synthesis 5 (Gcn5) or General control of amino-acid synthesis 5 like 2 (Gcn5l2). http://www.ncbi.nlm.nih.gov/gene/14534


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    1. On 2014 Aug 13, David Keller commented:

      Smoking reduces risk of PD, but increases risk of COPD and of vascular Parkinsonism

      It is well established that smoking is a major risk factor for COPD. Smoking has also been shown to reduce the risk of Parkinson disease (1), thought to be due to neuroprotection by nicotine (2). Therefore, based on the prior observed associations with smoking, one would expect the risk of PD to be lower in COPD patients than in patients with no smoking history. I propose that the unexpected association between COPD and PD may be due to misdiagnosis of vascular Parkinsonism as PD.

      Smoking is a major risk factor for COPD and for atherosclerotic vascular disease (ASVD). Parkinsonism can be caused by ASVD, in which case it is categorized as vascular Parkinsonism (VP), a disease distinct from classic neurodegenerative PD. VP would be expected to correlate directly with COPD, while PD should be inversely correlated with COPD, based on the known association of smoking with ASVD, and its inverse association with PD.

      COPD is expected to be associated with vascular Parkinsonism, but not with Parkinson's disease, based on the known relationships of these diseases with smoking. The results of this study would be consistent with these known associations if enough VP patients were misdiagnosed as having PD. I suggest that the data be re-examined to consider this possibility.

      Lastly, the authors refer to dementia as a neurodegenerative disease. Dementia is actually a symptom which can be caused by neurodegenerative diseases (such as Alzheimer's disease or dementia with Lewy bodies), atherosclerotic disease (as in multi-infarct vascular dementia), other disorders, or a combination thereof. It is incorrect to categorize dementia due to atherosclerotic infarctions as a "neurodegenerative disorder".

      References

      1: van der Mark M, Nijssen PC, Vlaanderen J, Huss A, Mulleners WM, Sas AM, van Laar T, Kromhout H, Vermeulen R. A case-control study of the protective effect of alcohol, coffee, and cigarette consumption on Parkinson disease risk: time-since-cessation modifies the effect of tobacco smoking. PLoS One. 2014 Apr 30;9(4):e95297. doi: 10.1371/journal.pone.0095297. eCollection 2014. PubMed PMID: 24788751; PubMed Central PMCID: PMC4005732.

      2: Ross GW, Petrovitch H. Current evidence for neuroprotective effects of nicotine and caffeine against Parkinson's disease. Drugs Aging. 2001;18(11):797-806. Review. PubMed PMID: 11772120.


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    1. On 2016 Dec 05, Anne Carpenter commented:

      Please note that there is a typo for the microscope's TexasRed filter, which is mentioned in the Supplemental Materials. It is listed as excitation/emission (562/642 nm) when it is actually (562/624 nm). This was confirmed with the screening center that performed the microscopy described in the paper.


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    2. On 2016 Dec 05, Anne Carpenter commented:

      As one of the senior authors on this paper, I report an error on page 14 of the Supporting Materials and Methods: the words "after cell fixation with 16% paraformaldehyde" should be replaced by "after cell fixation with 3.2% formaldehyde".


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    1. On 2016 Jan 06, Lydia Maniatis commented:

      This article finally clarified what the authors of this and similar papers mean by “biologically-generated” or “evolved” stimuli. Here are the relevant statements:

      The visual system achieves its goals on the basis of “the creation of light energy patterns whose frequency of occurrence tracks reproductive success...these patterns are “stimuli” ...Photon energy in the environment causes receptor cells in the retina to respond...It is only after the evolved apparatus of the eye collects, focuses, and selects a particular fraction of this energy into a biologically determined pattern that a stimulus exists...light stimuli are determined by a collaboration between physics and evolved biology.”

      Thus, Purves et al “stimulus” is simply the physiological state of the retina, which is contingent on incoming light that is focussed. I don't think anyone would argue with that. It acknowledges that the “stimulus” is connected with the physics of the world around us, specifically, the light impinging on the retina.

      However, this description of the visual stimulus does not in any way justify or explain the notion that the “frequency of occurrence” of these stimuli "tracks reproductive success.” The pattern of retinal stimulation changes with each movement of the eye, and the patterns, depending as they do on the chance arrangements of the environment and on the line of sight, on the time of day, etc, could fairly be described as “random.” Even if we could somehow define, categorise and track particular “patterns,” why should their frequency of occurrence track reproductive success? Also, since the slate, insofar as the frequency of occurrence of these light patterns is concerned, is wiped clean with every generation, how are these frequency distributions preserved?

      The repeated claims that the visual system can't use the stimulus to infer features of the physical world is contrdicted by the authors, who say that “the visual system does not take the measure of physical reality...that we readily assess with the instruments of physics.” In fact, we readily assess using our perception of the physical properties of the instruments of physics. In addition, the fact that focussing of light achieves a point to point correspondence between points on the retina and points in the world that reflected the light is suggestive of an attempt to infer the shapes and locations of actual physical objects.

      The claims about the inability of the v.s. to access properties of the physical world is made based on our perception of pictorial mimics of projections from real-world scenes. If I compare my perceptions of the color of objects in a naturally-lit real-life scene under inhomogeneous illumination, then my perception of the intrinsic surface properties of objects (e.g. reflectance, chromaticity) will appear quite reliable. If I then take a photo of that scene, and compare my perceptions of its surface properties to the actual properties of the photo surface, then, of course, errors all around. This doesn't justify denying the veridical outcome in the natural scene, or discounting it in accounts of how perception works.

      The methods are oddly weak. "Three hundred and eight high-resolution natural red–green–blue (RGB) images from The University of Texas at Austin “set 1” database (7) served as a proxy for human spectral experience.” [The sampling problem should speak for itself. The sample was collected by a different team with different priorities. We are not given a description of the images, or of the rationale with which they were collected. The lighting conditions are not controlled for before or after the fact. Perceptual effects are not tested. The claim that it is a proxy for human evolutionary experience is to be taken on faith. The argument of this paper hinges on this database.]


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    1. On 2014 Nov 24, Guillaume Filion commented:

      This article is one of the "CISCOM meta-analyses", which are very similar papers written by different authors. For more information about the CISCOM meta-analyses, check the blog post "A flurry of copycast on PubMed" at the following link http://blog.thegrandlocus.com/2014/10/a-flurry-of-copycats-on-pubmed


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    1. On 2014 Aug 04, MARK VRABEL commented:

      Good to see this article. My (librarian) contributions have been acknowledged on www.guidelines.gov; for example, "With the assistance of the Oncology Nursing Society (ONS) librarian" at http://www.guideline.gov/content.aspx?id=15702

      Mark Vrabel, MLS, AHIP, ELS Oncology Nursing Society twitter.com/ONSmark


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