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全基因组基因型-血清蛋白质组映射提供了对心血管代谢疾病易感性的跨种族差异的深入了解。

Genome-wide genotype-serum proteome mapping provides insights into the cross-ancestry differences in cardiometabolic disease susceptibility.

机构信息

School of Life Sciences, Fudan University, Shanghai, China.

School of Life Sciences, Westlake University, 310024, Hangzhou, China.

出版信息

Nat Commun. 2023 Feb 16;14(1):896. doi: 10.1038/s41467-023-36491-3.

Abstract

Identification of protein quantitative trait loci (pQTL) helps understand the underlying mechanisms of diseases and discover promising targets for pharmacological intervention. For most important class of drug targets, genetic evidence needs to be generalizable to diverse populations. Given that the majority of the previous studies were conducted in European ancestry populations, little is known about the protein-associated genetic variants in East Asians. Based on data-independent acquisition mass spectrometry technique, we conduct genome-wide association analyses for 304 unique proteins in 2,958 Han Chinese participants. We identify 195 genetic variant-protein associations. Colocalization and Mendelian randomization analyses highlight 60 gene-protein-phenotype associations, 45 of which (75%) have not been prioritized in Europeans previously. Further cross-ancestry analyses uncover key proteins that contributed to the differences in the obesity-induced diabetes and coronary artery disease susceptibility. These findings provide novel druggable proteins as well as a unique resource for the trans-ancestry evaluation of protein-targeted drug discovery.

摘要

鉴定蛋白质数量性状基因座(pQTL)有助于了解疾病的潜在机制,并发现有前途的药物干预靶点。对于最重要的一类药物靶点,遗传证据需要能够推广到不同的人群。鉴于之前的大多数研究都是在欧洲血统人群中进行的,因此对于东亚人的蛋白质相关遗传变异知之甚少。基于数据非依赖采集质谱技术,我们对 2958 名汉族参与者的 304 种独特蛋白质进行了全基因组关联分析。我们鉴定出 195 个遗传变异-蛋白质关联。共定位和孟德尔随机化分析突出了 60 个基因-蛋白质-表型关联,其中 45 个(75%)以前在欧洲人中没有得到优先考虑。进一步的跨血统分析揭示了导致肥胖引起的糖尿病和冠心病易感性差异的关键蛋白质。这些发现为药物靶点的药物发现提供了新的可成药蛋白质,以及一个独特的跨血统评估资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a6dc/9935862/0c945c26aa44/41467_2023_36491_Fig1_HTML.jpg

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