Large scale plasma proteomics identifies novel proteins and protein networks associated with heart failure development

Author:

Shah Amil M.ORCID,Myhre Peder L.,Arthur VictoriaORCID,Dorbala Pranav,Rasheed HumairaORCID,Buckley Leo F.,Claggett Brian,Liu Guning,Ma Jianzhong,Nguyen Ngoc Quynh,Matsushita Kunihiro,Ndumele Chiadi,Tin AdrienneORCID,Hveem Kristian,Jonasson ChristianORCID,Dalen Håvard,Boerwinkle Eric,Hoogeveen Ron C.,Ballantyne ChristieORCID,Coresh JosefORCID,Omland Torbjørn,Yu BingORCID

Abstract

AbstractHeart failure (HF) causes substantial morbidity and mortality but its pathobiology is incompletely understood. The proteome is a promising intermediate phenotype for discovery of novel mechanisms. We measured 4877 plasma proteins in 13,900 HF-free individuals across three analysis sets with diverse age, geography, and HF ascertainment to identify circulating proteins and protein networks associated with HF development. Parallel analyses in Atherosclerosis Risk in Communities study participants in mid-life and late-life and in Trøndelag Health Study participants identified 37 proteins consistently associated with incident HF independent of traditional risk factors. Mendelian randomization supported causal effects of 10 on HF, HF risk factors, or left ventricular size and function, including matricellular (e.g. SPON1, MFAP4), senescence-associated (FSTL3, IGFBP7), and inflammatory (SVEP1, CCL15, ITIH3) proteins. Protein co-regulation network analyses identified 5 modules associated with HF risk, two of which were influenced by genetic variants that implicated trans hotspots within the VTN and CFH genes.

Funder

U.S. Department of Health & Human Services | NIH | National Heart, Lung, and Blood Institute

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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