He analysed the flow of blood around the heart, makingthe world’s first post-mortem diagnosis of arteriosclerosis, and worked outhow the aortic valve manages the turbulence of rushing blood.
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- Jul 2025
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Local file Local file
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- Jan 2025
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www.youtube.com www.youtube.com
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for - Youtube - book review - Reviewing "The Brain Abstracted - Simplification in the History and Philosophy of Neuroscience" - M. Chirimuuta - Youtube channel: Philosophy of Psychiatric Diagnoses - 2025 Jan 23
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I think the book is fantastic I'm now going to outlined review of a book and then at the end briefly point out some potential implications for psychiatric diagnosis and neurodiversity
for - implications of book "The Brain Abstracted" for neurodiversity - SOURCE - Youtube - book review - Reviewing "The Brain Abstracted - Simplification in the History and Philosophy of Neuroscience" - M. Chirimuuta - Youtube channel: Philosophy of Psychiatric Diagnoses - 2025 Jan 23
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- Youtube - book review - Reviewing "The Brain Abstracted - Simplification in the History and Philosophy of Neuroscience" - M. Chirimuuta - Youtube channel: Philosophy of Psychiatric Diagnoses - 2025 Jan 23
- implications of book "The Brain Abstracted" for neurodiversity - SOURCE - Youtube - book review - Reviewing "The Brain Abstracted - Simplification in the History and Philosophy of Neuroscience" - M. Chirimuuta - Youtube channel: Philosophy of Psychiatric Diagnoses - 2025 Jan 23
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- Oct 2024
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journals.lww.com journals.lww.com
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Disease: mild haemophilia A, influencing VWF levels
Patient: 20 yo, Female
Variant1: F8 NM_000132.3: c.1127T>G: p. Val376Gly (Exon 8, current clinvar interpretation not available)
Variant 2: F8 NM_000132.3: c.3780C>G: p. Asp1260Glu (Exon 14, current ClinVar interpretation is benign)
Variant 3: VWF NM_000552.5: c.1415A>G:p.His484Arg (Exon 13, current ClinVar interpretation is Benign/likely Benign)
Variant 4: VWF NM_000552.5: c.2365A>G:p.Thr789Ala (Exon 18, current ClinVar interpretation is Benign/ likely Benign)
Variant 5: VWF NM_000552.5: c.2771G>A:p.Arg924Gln (Exon 21, current ClinVar interpretation is conflicting interpretations of pathogenicity (VUS-3)(Benign-4)(Likely benign-1))
Variant 6: VWF NM_000552.5: c.4141A>G:p.Thr1381Ala (Exon 28, current ClinVar interpretation is Benign/ Likely Benign)
Variant 7: VWF NM_000552.5: c.6532G>T:p.Ala2178Ser (Exon 37, Conflicting interpretations of pathogenicity: (VUS-1) (Likely Benign-1))
Variant 8: F5 NM_000130.5: c.2773A>G:p.Lys925Glu (Exon 13, current ClinVar interpretation is Benign/Likely Benign)
Variant 9: F5 NM_000130.5: c.2594A>G:p.His865Arg (Exon 13, current ClinVar interpretation is Benign/Likely Benign)
Variant 10: F5 NM_000130.5: c.2573A>G:p.Lys858Arg (Exon 13, Conflicting interpretations of pathogenicity: (VUS-1) (Benign-2)(Likely Benign-1))
Variant 11: F5 NM_000130.5: c.5290A>G:p.Met1764Val (Exon 16, Conflicting interpretations of pathogenicity: (VUS-1) (Benign-2)(Likely Benign-1))
Variant 12: F13A1 NM_000129.4: c.103G>T:p.Val35Leu (Exon 2, Conflicting interpretations of pathogenicity: (VUS-1) (Benign-3))
Variant notes: All are heterozygous
Both variants in F8 are linked to reports associated with haemophilia, though second variant is considered benign.
Phenotypes: History of bleeding (Heavy mentrual bleeding since menarche)(Treated with transdermal oestrogen and Levonorgestel), iron deficiency anaemia. High Janssen score for pictorial blood assessment. Gum bleeding lasting longer than 10 minutes(Treated with local application of tranexamic acid), recurrent nosebleeds, high score for ISTH and BAT assessments. Decrease in VWF:Ag ratio, VWF:CB ratio decreased, VWF: GPIbR ratio decreased
Family: Maternal grandfather possibly haemophiliac, mother asymptomatic
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