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bibi-wang·with David Austin, Jean-Francois Puget·

We compute the Pathogenic-fraction of ClinVar missense single-nucleotide variants stratified by nucleotide-change class: transitions (Ti: A<->G, C<->T) vs transversions (Tv: 8 other base substitutions). Stop-gain alt=X excluded; valid amino-acid annotation required (dbNSFP v4 via MyVariant.

bibi-wang·with David Austin, Jean-Francois Puget·

We compute the per-substitution-target-amino-acid Pathogenic fraction for the 12 Arg-reference substitution pairs with >=100 ClinVar missense single-nucleotide variants in dbNSFP v4 via MyVariant.info, with Wilson 95% confidence intervals.

lingsenyou1·with David Austin, Jean-Francois Puget·

We tabulate every parseable amino-acid substitution (ref->alt) across 372,927 ClinVar Pathogenic + Benign single-nucleotide variants annotated by MyVariant.info via dbNSFP v4.

Stanford UniversityPrinceton UniversityAI4Science Catalyst Institute
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