Identifying Susceptibility Genes and Shared Genetic Architecture for Longevity and Muscle Weakness
Yilong Lin, Yun Zhang, Shengjie Lin, Songsong Wang, Zhiqiang Que, Yue Zhang, Jing She, Ruidan Zhao, Jiawei Chen, Anqi Qiu, Shinan Wu, Ruiqin Yang, Liyi Zhang, Qingmo Yang

TL;DR
This study identifies genes linked to longevity and muscle weakness, revealing shared genetic factors that could help promote healthy aging.
Contribution
The study identifies novel susceptibility genes and shared genetic architecture between longevity and muscle weakness using large-scale GWAS and multi-tissue analysis.
Findings
APOC1 and TOMM40 are associated with longevity, while DYM and TGFA are linked to muscle weakness.
A significant negative genetic correlation exists between longevity and muscle weakness.
Pleiotropic genes like PVRL2, PPP1R9A, and the TOMM40/APOE/APOC1 cluster influence both traits.
Abstract
Longevity and muscle strength are heritable traits, and age‐related muscle weakness is a major contributor to disability in older adults. However, the susceptibility genes and shared genetic mechanisms underlying lifespan and sarcopenia remain unclear. This study aimed to identify genes associated with longevity and muscle weakness and to characterize their shared genetic architecture. We integrated the largest genome‐wide association studies (GWAS) on longevity (age > 90th: n = 11 262 cases; age > 99th: n = 3484 cases) and muscle weakness (European Working Group on Sarcopenia in Older People (EWGSOP): n = 48 596 cases; Foundation for the National Institutes of Health (FNIH): n = 20 335 cases) with Genotype‐Tissue Expression (GTEx) v8 multi‐tissue expression quantitative trait locus (eQTL) data. Gene–trait associations were evaluated using multi‐tissue and single‐tissue TWAS, and…
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Taxonomy
TopicsGenetics, Aging, and Longevity in Model Organisms · Genetic Associations and Epidemiology · Nutrition and Health in Aging
