Phenotypic Findings Associated with Variation in Elastin

Anne E Justice, Melissa A Kelly, Gary Bellus, Joshua D Green, Raza Zaidi, Taylor Kerrins, Navya Josyula, Teresa Romeo Luperchio, Beth A Kozel, Marc S Williams
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引用次数: 0

Abstract

Variation in the elastin gene (ELN) may contribute to connective tissue disease beyond the known disease associations of Supravalvar Aortic Stenosis and Cutis Laxa. Exome data from MyCode Community Health Initiative participants were analyzed for ELN rare variants (mean allele frequency <1%, not currently annotated as benign). Participants with variants of interest underwent phenotyping by dual chart review using a standardized abstraction tool. Additionally, all rare variants that met inclusion criteria were collapsed intoan ELN gene burden score to perform a Phenome-wide Association Study (PheWAS). Two hundred and ninety-six eligible participants with relevant ELN variants were identified from 184,293 MyCode participants. One hundred and three of 254 living participants (41%) met phenotypic criteria, most commonly aortic hypoplasia, arterial dilation, aneurysm, and dissection, and connective tissue abnormalities. ELN variation was significantly (P <2.8x10-5) associated with "arterial dissection" in the PheWAS and two connective tissue Phecodes approached significance. Variation in ELN is associated with connective tissue pathology beyond classic phenotypes.
与弹性蛋白变异相关的表型结果
弹性蛋白基因(ELN)的变异可能会导致结缔组织疾病,而不局限于已知的主动脉瓣上狭窄症(Supravalvar Aortic Stenosis)和皮肤松弛症(Cutis Laxa)。对 MyCode Community HealthInitiative 参与者的外显子组数据进行了分析,以发现 ELN 罕见变异(平均等位基因频率为 1%,目前未注明为良性)。通过使用标准化摘要工具进行双重病历审查,对具有相关变异的参与者进行了表型分析。此外,所有符合纳入标准的罕见变异都被归入 ELN 基因负担评分,以进行全表型关联研究(Phenome-wide Association Study,PheWAS)。从 184,293 名 MyCode 参与者中确定了 26 名具有相关 ELN 变异的合格参与者。254 名在世参与者中有 103 人(41%)符合表型标准,其中最常见的是主动脉发育不良、动脉扩张、动脉瘤和夹层以及结缔组织异常。ELN变异与PheWAS中的 "动脉夹层 "有明显相关性(P<2.8x10-5),两个结缔组织Phecodes接近显著性。ELN的变异与结缔组织病理学的关系超出了传统的表型。
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