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计算得出的瓣环直径揭示了二尖瓣功能和疾病的遗传决定因素。

Computational estimates of annular diameter reveal genetic determinants of mitral valve function and disease.

机构信息

Department of Pediatrics and.

Division of Cardiovascular Medicine, Stanford University School of Medicine, Stanford, California, USA.

出版信息

JCI Insight. 2022 Feb 8;7(3):e146580. doi: 10.1172/jci.insight.146580.

Abstract

The fibrous annulus of the mitral valve plays an important role in valvular function and cardiac physiology, while normal variation in the size of cardiovascular anatomy may share a genetic link with common and rare disease. We derived automated estimates of mitral valve annular diameter in the 4-chamber view from 32,220 MRI images from the UK Biobank at ventricular systole and diastole as the basis for GWAS. Mitral annular dimensions corresponded to previously described anatomical norms, and GWAS inclusive of 4 population strata identified 10 loci, including possibly novel loci (GOSR2, ERBB4, MCTP2, MCPH1) and genes related to cardiac contractility (BAG3, TTN, RBFOX1). ATAC-Seq of primary mitral valve tissue localized multiple variants to regions of open chromatin in biologically relevant cell types and rs17608766 to an algorithmically predicted enhancer element in GOSR2. We observed strong genetic correlation with measures of contractility and mitral valve disease and clinical correlations with heart failure, cerebrovascular disease, and ventricular arrhythmias. Polygenic scoring of mitral valve annular diameter in systole was predictive of risk mitral valve prolapse across 4 cohorts. In summary, genetic and clinical studies of mitral valve annular diameter revealed genetic determinants of mitral valve biology, while highlighting clinical associations. Polygenic determinants of mitral valve annular diameter may represent an independent risk factor for mitral prolapse. Overall, computationally estimated phenotypes derived at scale from medical imaging represent an important substrate for genetic discovery and clinical risk prediction.

摘要

二尖瓣的纤维性瓣环在瓣膜功能和心脏生理中起着重要作用,而心血管解剖结构的正常变化可能与常见和罕见疾病有遗传联系。我们从英国生物库的 32220 份 MRI 图像中,在心室收缩期和舒张期自动估计了二尖瓣瓣环直径在四腔心视图中的大小,以此作为 GWAS 的基础。二尖瓣瓣环尺寸与之前描述的解剖学标准相对应,包含 4 个人群分层的 GWAS 确定了 10 个位点,包括可能的新位点(GOSR2、ERBB4、MCTP2、MCPH1)和与心脏收缩性相关的基因(BAG3、TTN、RBFOX1)。原发性二尖瓣组织的 ATAC-Seq 将多个变体定位到生物相关细胞类型的开放染色质区域,以及 rs17608766 到 GOSR2 中算法预测的增强子元件。我们观察到与收缩性和二尖瓣疾病的测量值以及与心力衰竭、脑血管疾病和室性心律失常的临床相关性具有很强的遗传相关性。收缩期二尖瓣瓣环直径的多基因评分在 4 个队列中对风险性二尖瓣脱垂具有预测性。总之,对二尖瓣瓣环直径的遗传和临床研究揭示了二尖瓣生物学的遗传决定因素,同时强调了临床关联。二尖瓣瓣环直径的多基因决定因素可能是二尖瓣脱垂的一个独立危险因素。总的来说,从医学成像中大规模计算得出的表型代表了遗传发现和临床风险预测的重要基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/983e/8855800/ecf01a825bd4/jciinsight-7-146580-g268.jpg

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