表观基因组
效应器
转录组
骨关节炎
生物信息学
蛋白质组
疾病
医学
表观遗传学
生物
计算生物学
遗传学
内科学
基因表达
病理
基因
细胞生物学
DNA甲基化
替代医学
作者
Konstantinos Hatzikotoulas,Lorraine Southam,Lilja Stefánsdóttir,Cindy G. Boer,Merry‐Lynn McDonald,J. Patrick Pett,Young‐Chan Park,Margo Tuerlings,Rick Mulders,Andrei Barysenka,Ana Luiza Arruda,Vinicius Tragante,Alison Rocco,Norbert Bittner,Shibo Chen,Susanne Horn,Vinodh Srinivasasainagendra,Ken To,Georgia Katsoula,Peter Kreitmaier
出处
期刊:Nature
[Nature Portfolio]
日期:2025-04-09
卷期号:641 (8065): 1217-1224
被引量:44
标识
DOI:10.1038/s41586-025-08771-z
摘要
Osteoarthritis is the third most rapidly growing health condition associated with disability, after dementia and diabetes1. By 2050, the total number of patients with osteoarthritis is estimated to reach 1 billion worldwide2. As no disease-modifying treatments exist for osteoarthritis, a better understanding of disease aetiopathology is urgently needed. Here we perform a genome-wide association study meta-analyses across up to 489,975 cases and 1,472,094 controls, establishing 962 independent associations, 513 of which have not been previously reported. Using single-cell multiomics data, we identify signal enrichment in embryonic skeletal development pathways. We integrate orthogonal lines of evidence, including transcriptome, proteome and epigenome profiles of primary joint tissues, and implicate 700 effector genes. Within these, we find rare coding-variant burden associations with effect sizes that are consistently higher than common frequency variant associations. We highlight eight biological processes in which we find convergent involvement of multiple effector genes, including the circadian clock, glial-cell-related processes and pathways with an established role in osteoarthritis (TGFβ, FGF, WNT, BMP and retinoic acid signalling, and extracellular matrix organization). We find that 10% of the effector genes express a protein that is the target of approved drugs, offering repurposing opportunities, which can accelerate translation.
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