FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4365998049> ?p ?o ?g. }

• W4365998049 endingPage "740" @default.
• W4365998049 startingPage "722" @default.
• W4365998049 abstract "Coronary artery disease (CAD) is a pandemic disease where up to half of the risk is explained by genetic factors. Advanced insights into the genetic basis of CAD require deeper understanding of the contributions of different cell types, molecular pathways, and genes to disease heritability. Here, we investigate the biological diversity of atherosclerosis-associated cell states and interrogate their contribution to the genetic risk of CAD by using single-cell and bulk RNA sequencing (RNA-seq) of mouse and human lesions. We identified 12 disease-associated cell states that we characterized further by gene set functional profiling, ligand-receptor prediction, and transcription factor inference. Importantly, Vcam1+ smooth muscle cell state genes contributed most to SNP-based heritability of CAD. In line with this, genetic variants near smooth muscle cell state genes and regulatory elements explained the largest fraction of CAD-risk variance between individuals. Using this information for variant prioritization, we derived a hybrid polygenic risk score (PRS) that demonstrated improved performance over a classical PRS. Our results provide insights into the biological mechanisms associated with CAD risk, which could make a promising contribution to precision medicine and tailored therapeutic interventions in the future." @default.
• W4365998049 created "2023-04-17" @default.
• W4365998049 creator A5002650985 @default.
• W4365998049 creator A5005664319 @default.
• W4365998049 creator A5011313978 @default.
• W4365998049 creator A5012959772 @default.
• W4365998049 creator A5014220812 @default.
• W4365998049 creator A5014513326 @default.
• W4365998049 creator A5019463144 @default.
• W4365998049 creator A5034050108 @default.
• W4365998049 creator A5038506999 @default.
• W4365998049 creator A5039535400 @default.
• W4365998049 creator A5040157542 @default.
• W4365998049 creator A5040452430 @default.
• W4365998049 creator A5045671475 @default.
• W4365998049 creator A5048635182 @default.
• W4365998049 creator A5057736898 @default.
• W4365998049 creator A5059968020 @default.
• W4365998049 creator A5061617676 @default.
• W4365998049 creator A5075082700 @default.
• W4365998049 creator A5081986241 @default.
• W4365998049 date "2023-05-01" @default.
• W4365998049 modified "2023-10-17" @default.
• W4365998049 title "Dissecting the polygenic basis of atherosclerosis via disease-associated cell state signatures" @default.
• W4365998049 cites W1844405070 @default.
• W4365998049 cites W1924112666 @default.
• W4365998049 cites W2014677321 @default.
• W4365998049 cites W2022779537 @default.
• W4365998049 cites W2026662206 @default.
• W4365998049 cites W2076522499 @default.
• W4365998049 cites W2099085143 @default.
• W4365998049 cites W2156634381 @default.
• W4365998049 cites W2169456326 @default.
• W4365998049 cites W2171705978 @default.
• W4365998049 cites W2171808845 @default.
• W4365998049 cites W2214074259 @default.
• W4365998049 cites W2238851414 @default.
• W4365998049 cites W2332292689 @default.
• W4365998049 cites W2558476889 @default.
• W4365998049 cites W2580419588 @default.
• W4365998049 cites W2581330857 @default.
• W4365998049 cites W2616922646 @default.
• W4365998049 cites W2617149455 @default.
• W4365998049 cites W2735404270 @default.
• W4365998049 cites W2775393828 @default.
• W4365998049 cites W2777667999 @default.
• W4365998049 cites W2791863121 @default.
• W4365998049 cites W2795181515 @default.
• W4365998049 cites W2803878103 @default.
• W4365998049 cites W2892012404 @default.
• W4365998049 cites W2895486342 @default.
• W4365998049 cites W2898549090 @default.
• W4365998049 cites W2921330004 @default.
• W4365998049 cites W2942610007 @default.
• W4365998049 cites W2944545583 @default.
• W4365998049 cites W2949177718 @default.
• W4365998049 cites W2949754140 @default.
• W4365998049 cites W2950099124 @default.
• W4365998049 cites W2955417896 @default.
• W4365998049 cites W2958615822 @default.
• W4365998049 cites W2966605790 @default.
• W4365998049 cites W2970727076 @default.
• W4365998049 cites W2974827020 @default.
• W4365998049 cites W2976681669 @default.
• W4365998049 cites W2979167769 @default.
• W4365998049 cites W2984828313 @default.
• W4365998049 cites W2988296254 @default.
• W4365998049 cites W2992151131 @default.
• W4365998049 cites W2996535147 @default.
• W4365998049 cites W3002402252 @default.
• W4365998049 cites W3010766518 @default.
• W4365998049 cites W3027019670 @default.
• W4365998049 cites W3030739213 @default.
• W4365998049 cites W3030835293 @default.
• W4365998049 cites W3042532729 @default.
• W4365998049 cites W3042705713 @default.
• W4365998049 cites W3088819072 @default.
• W4365998049 cites W3089136059 @default.
• W4365998049 cites W3090627945 @default.
• W4365998049 cites W3110255422 @default.
• W4365998049 cites W3111554464 @default.
• W4365998049 cites W3120458719 @default.
• W4365998049 cites W3126364712 @default.
• W4365998049 cites W3162108567 @default.
• W4365998049 cites W3163167535 @default.
• W4365998049 cites W3164307931 @default.
• W4365998049 cites W3184729641 @default.
• W4365998049 cites W3185145116 @default.
• W4365998049 cites W3203496375 @default.
• W4365998049 cites W3210601686 @default.
• W4365998049 cites W3214158901 @default.
• W4365998049 cites W3216708429 @default.
• W4365998049 cites W4214697101 @default.
• W4365998049 cites W4225826665 @default.
• W4365998049 cites W4226027293 @default.
• W4365998049 cites W4289261048 @default.
• W4365998049 cites W4310766578 @default.
• W4365998049 cites W4317390883 @default.

• next