Proteomic aging clock predicts mortality and risk of common age-related diseases in diverse populations

Argentieri, M. Austin; Xiao, Sihao; Bennett, Derrick; Winchester, Laura; Nevado‐Holgado, Alejo; Ghose, Upamanyu; Albukhari, Ashwag; Yao, Pang; Mazidi, Mohsen; Lv, Jun; Millwood, Iona Y.; Fry, Hannah; Rodosthenous, Rodosthenis S.; Partanen, Jukka; Zheng, Zhili; Kurki, Mitja; Daly, Mark J.; Palotie, Aarno; Adams, Cassandra; Li, Liming; Clarke, Robert; Amin, Najaf; Chen, Zhengming; Duijn, Cornelia M. van

doi:10.1038/s41591-024-03164-7

articleNature MedicineAug 8, 2024HYBRID OA

Proteomic aging clock predicts mortality and risk of common age-related diseases in diverse populations

MAM. Austin Argentieri SXSihao Xiao DBDerrick Bennett LWLaura Winchester ANAlejo Nevado‐Holgado

Broad Institute · University of Oxford · +6 more institutions

PubMed

Indexed incrossrefpubmed

Abstract

Circulating plasma proteins play key roles in human health and can potentially be used to measure biological age, allowing risk prediction for age-related diseases, multimorbidity and mortality. Here we developed a proteomic age clock in the UK Biobank (n = 45,441) using a proteomic platform comprising 2,897 plasma proteins and explored its utility to predict major disease morbidity and mortality in diverse populations. We identified 204 proteins that accurately predict chronological age (Pearson r = 0.94) and found that proteomic aging was associated with the incidence of 18 major chronic diseases (including diseases of the heart, liver, kidney and lung, diabetes, neurodegeneration and cancer), as well as…

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260

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FWCI: 75.64
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24

Topics & keywords

Topics

Keywords

Biology
Gerontology
Medicine
Demography
Bioinformatics

UN Sustainable Development Goals

Good health and well-being

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Funding

MR
Medical Research Council
Awards: MC_PC_14135, MC_UU_00017/1