Ron Do

924 posts

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Ron Do

Ron Do

@DoGenetics

Human Geneticist. Data Scientist. Professor @IcahnMountSinai @BronfmanInst

New York, NY Se unió Nisan 2015
831 Siguiendo1.1K Seguidores
Ron Do retuiteado
Jonathan Pritchard
Jonathan Pritchard@jkpritch·
Modern GWAS can identify 1000s of significant hits but it can be hard to turn this into biological insight. I'm excited to share our new work combining genetic associations and Perturb-seq to build interpretable causal graphs, out today in @Nature:
Jonathan Pritchard tweet media
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Ron Do retuiteado
Nature Reviews Genetics
Nature Reviews Genetics@NatureRevGenet·
Successful drug development depends on identifying effective targets and optimizing drug design and clinical trial strategies. The authors review computational strategies, including ML, for integrating genetics into pharmaceutical pipelines go.nature.com/43VZslH
Nature Reviews Genetics tweet media
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Marios Georgakis
Marios Georgakis@MariosGeorgakis·
A nice weekend read on methods for prioritizing drug targets for complex diseases using human genomic data👇
Marios Georgakis tweet media
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Loïc Yengo
Loïc Yengo@LoicYengo·
We are pleased to announce that our new study explaining the missing heritability of many phenotypes using WGS data from ~347,000 UK Biobank participants has just been published in @Nature. Please check out our manuscript here: nature.com/articles/s4158….
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Iain S. Forrest, MD-PhD
Iain S. Forrest, MD-PhD@IainSForrest·
🚨“Pathogenic” genetic variant does NOT = guaranteed disease 🚨 Yet, doctors and patients are still left to decide what to do with the label… In our new @NatureGenet perspective, we explain why this is and how we can improve genetic risk interpretation🧵
Iain S. Forrest, MD-PhD tweet media
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Ron Do
Ron Do@DoGenetics·
11/ This approach is scalable and can be applied to many different types of variants and diseases. It demonstrates how integrating ML + EHR + genomics can move us from categorical pathogenicity labels toward more data-driven and quantitative penetrance estimates. /end
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Ron Do
Ron Do@DoGenetics·
10/ Applications include: - improving variant classification - guiding clinical genetics & counseling - prioritizing variants for research - personalized disease risk stratification.
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