Bidirectional Risk Modulator and Modifier Variant of Dilated and Hypertrophic Cardiomyopathy in BAG3

IF 14.8 1区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS JAMA cardiology Pub Date : 2024-11-13 DOI:10.1001/jamacardio.2024.3547
Joseph Park, Michael G. Levin, David Zhang, Nosheen Reza, Jonathan O. Mead, Eric D. Carruth, Melissa A. Kelly, Alex Winters, Colleen M. Kripke, Renae L. Judy, Scott M. Damrauer, Anjali T. Owens, Lisa Bastarache, Anurag Verma, Daniel D. Kinnamon, Ray E. Hershberger, Marylyn D. Ritchie, Daniel J. Rader
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Abstract

ImportanceThe genetic factors that modulate the reduced penetrance and variable expressivity of heritable dilated cardiomyopathy (DCM) are largely unknown. BAG3 genetic variants have been implicated in both DCM and hypertrophic cardiomyopathy (HCM), nominating BAG3 as a gene that harbors potential modifier variants in DCM.ObjectiveTo interrogate the clinical traits and diseases associated with BAG3 coding variation.Design, Setting, and ParticipantsThis was a cross-sectional study in the Penn Medicine BioBank (PMBB) enrolling patients of the University of Pennsylvania Health System’s clinical practice sites from 2014 to 2023. Whole-exome sequencing (WES) was linked to electronic health record (EHR) data to associate BAG3 coding variants with EHR phenotypes. This was a health care population-based study including individuals of European and African genetic ancestry in the PMBB with WES linked to EHR phenotypes, with replication studies in BioVU, UK Biobank, MyCode, and DCM Precision Medicine Study.ExposuresCarrier status for BAG3 coding variants.Main Outcomes and MeasuresAssociation of BAG3 coding variation with clinical diagnoses, echocardiographic traits, and longitudinal outcomes.ResultsIn PMBB (n = 43 731; median [IQR] age, 65 [50-76] years; 21 907 female [50.1%]), among 30 324 European and 11 198 African individuals, the common C151R variant was associated with decreased risk for DCM (odds ratio [OR], 0.85; 95% CI, 0.78-0.92) and simultaneous increased risk for HCM (OR, 1.59; 95% CI, 1.25-2.02), which was confirmed in the replication cohorts. C151R carriers exhibited improved longitudinal outcomes compared with noncarriers as assessed by age at death (hazard ratio [HR], 0.85; 95% CI, 0.74-0.96; median [IQR] age, 71.8 [63.1-80.7] in carriers and 70.3 [61.6-79.2] in noncarriers) and heart transplant (HR, 0.81; 95% CI, 0.66-0.99; median [IQR] age, 56.7 [46.1-63.1] in carriers and 55.6 [45.2-62.9] in noncarriers). C151R was associated with reduced risk of DCM (OR, 0.42; 95% CI, 0.24-0.74) and heart failure (OR, 0.27; 95% CI, 0.14-0.50) among individuals harboring truncating TTN variants in exons with high cardiac expression (n = 358).Conclusions and RelevanceBAG3 C151R was identified as a bidirectional modulator of risk along the DCM-HCM spectrum, as well as an important genetic modifier variant in TTN-mediated DCM. This work expands on the understanding of the etiology and penetrance of DCM, suggesting that BAG3 C151R is an important genetic modifier variant contributing to the variable expressivity of DCM, warranting further exploration of its mechanisms and of genetic modifiers in DCM more broadly.
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BAG3 中扩张型和肥厚型心肌病的双向风险调节器和调节变异体
重要性调节遗传性扩张型心肌病(DCM)的低渗透性和多变表达性的遗传因素在很大程度上尚属未知。BAG3基因变异与扩张型心肌病和肥厚型心肌病(HCM)都有关联,因此BAG3被认为是扩张型心肌病潜在的修饰变异基因。目的探讨与BAG3编码变异相关的临床特征和疾病。全外显子组测序(WES)与电子健康记录(EHR)数据相连接,以便将 BAG3 编码变异与电子健康记录表型联系起来。这是一项基于医疗保健人群的研究,包括 PMBB 中的欧洲和非洲遗传血统个体,WES 与 EHR 表型相关联,并在 BioVU、UK Biobank、MyCode 和 DCM Precision Medicine Study 中进行了复制研究。结果在30 324名欧洲人和11 198名非洲人的PMBB(n = 43 731;中位数[IQR]年龄,65 [50-76]岁;21 907名女性[50.1%])中,常见的C151R变异与DCM风险降低(几率比[OR],0.85;95% CI,0.78-0.92)和HCM风险增加(OR,1.59;95% CI,1.25-2.02)相关,这在复制队列中得到了证实。根据死亡年龄评估,C151R 携带者的纵向预后比非携带者有所改善(危险比 [HR],0.85;95% CI,0.74-0.96;携带者的中位 [IQR] 年龄为 71.8 [63.1-80.7],非携带者为 70.3 [61.6-79.2])和心脏移植(HR,0.81;95% CI,0.66-0.99;中位数[IQR]年龄,携带者为 56.7 [46.1-63.1],非携带者为 55.6 [45.2-62.9])。在心脏高表达外显子(n = 358)中携带截短 TTN 变异的个体中,C151R 与 DCM(OR,0.42;95% CI,0.24-0.74)和心力衰竭(OR,0.27;95% CI,0.14-0.50)风险降低相关。这项工作拓展了人们对 DCM 病因学和渗透性的认识,表明 BAG3 C151R 是导致 DCM 表现性多变的一个重要遗传修饰变体,值得进一步探索其机制以及更广泛的 DCM 遗传修饰变体。
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来源期刊
JAMA cardiology
JAMA cardiology Medicine-Cardiology and Cardiovascular Medicine
CiteScore
45.80
自引率
1.70%
发文量
264
期刊介绍: JAMA Cardiology, an international peer-reviewed journal, serves as the premier publication for clinical investigators, clinicians, and trainees in cardiovascular medicine worldwide. As a member of the JAMA Network, it aligns with a consortium of peer-reviewed general medical and specialty publications. Published online weekly, every Wednesday, and in 12 print/online issues annually, JAMA Cardiology attracts over 4.3 million annual article views and downloads. Research articles become freely accessible online 12 months post-publication without any author fees. Moreover, the online version is readily accessible to institutions in developing countries through the World Health Organization's HINARI program. Positioned at the intersection of clinical investigation, actionable clinical science, and clinical practice, JAMA Cardiology prioritizes traditional and evolving cardiovascular medicine, alongside evidence-based health policy. It places particular emphasis on health equity, especially when grounded in original science, as a top editorial priority.
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