电子健康记录生物库队列再现了重症成人 MUC5B 启动子多态性与 ARDS 之间的关联。

Vern Eric Kerchberger, Joel Brennan McNeil, Neil Zheng, Diana Chang, Carrie Rosenberger, Angela J Rogers, Julie A Bastarache, QiPing Feng, WeiQi Wei, Lorraine B Ware
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引用次数: 0

摘要

背景:与传统研究设计相比,与电子健康记录(EHR)相连的大型人群 DNA 生物库在识别 ARDS 遗传驱动因素方面可能具有优势:研究设计与方法:我们分析了一家学术医疗中心的两个基因分型队列:一项针对重症成人的前瞻性生物标记物研究(VALID 队列)和一个去标识化电子病历生物库(BioVU)中的住院参与者。在 VALID 和 BioVU 中,ARDS 状态分别由临床医生-调查员审查和电子病历衍生算法(EHR-ARDS)评估。我们检测了每个队列中 MUC5B 启动子多态性(rs35705950)与 ARDS/EHR-ARDS 发生之间的关联:VALID共纳入2795名患者,年龄为55 [43,66](中位数[IQR])岁,其中718人(25.7%)发生了ARDS。BioVU 纳入了 9025 名住院参与者,年龄为 60 [48, 70] 岁,有 1056 人(11.7%)发生了 EHR-ARDS。在 VALID 中,我们观察到年龄和 rs35705950 之间对 ARDS 风险有明显的交互作用:在老年患者中,rs35705950 与 ARDS 风险的增加相关(OR:1.44;95%CI 1.08-1.92;p=0.012),而在年轻患者中,这种效应减弱(OR:0.84;95%CI:0.62-1.14;p=0.26)。在 BioVU 中,在所有参与者中,rs35705950 与 EHR-ARDS 风险增加有关(OR:1.20;95%CI:1.00-1.43;p=0.043),这种关系不因年龄而异。在需要机械通气的 BioVU 参与者中,该多态性还与更严重的氧合障碍有关:在两组高危住院成人中,MUC5B启动子多态性与ARDS有关。虽然仅在前瞻性生物标志物队列中观察到与年龄相关的效应改变,但 EHR 队列发现 MUC5B 与 ARDS 风险之间存在一致的关联,与年龄无关,而且与氧合功能障碍存在新的关联。我们的研究强调了电子病历生物库在开展精准医疗 ARDS 研究方面的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Electronic health record biobank cohort recapitulates an association between the MUC5B promoter polymorphism and ARDS in critically ill adults.
Background: Large population-based DNA biobanks linked to electronic health records (EHRs) may provide advantages over traditional study designs for identifying genetic drivers of ARDS. Research Question: Can ARDS be identified in an EHR biobank, and can this approach validate a previously reported genetic risk factor for ARDS? Study Design and Methods: We analyzed two genotyped cohorts from one academic medical center: a prospective biomarker study of critically ill adults (VALID cohort), and hospitalized participants in a de-identified EHR biobank (BioVU). ARDS status was assessed by clinician-investigator review in VALID and an EHR-derived algorithm in BioVU (EHR-ARDS). We tested the association between the MUC5B promoter polymorphism (rs35705950) with development of ARDS/EHR-ARDS in each cohort. Results: In VALID, 2,795 patients were included, age was 55 [43, 66] (median [IQR]) years, and 718 (25.7%) developed ARDS. In BioVU, 9,025 hospitalized participants were included, age was 60 [48, 70] , and 1,056 (11.7%) developed EHR-ARDS. We observed a significant interaction between age and rs35705950 on ARDS risk in VALID: in older patients rs35705950 was associated with increased ARDS risk (OR: 1.44; 95%CI 1.08-1.92; p=0.012) whereas among younger patients this effect was attenuated (OR: 0.84; 95%CI: 0.62-1.14; p=0.26). In BioVU, rs35705950 was associated with increased risk for EHR-ARDS among all participants (OR: 1.20; 95%CI: 1.00-1.43, p=0.043) and this relationship did not vary by age. The polymorphism was also associated with more severe oxygenation impairment among BioVU participants who required mechanical ventilation. Interpretation: The MUC5B promoter polymorphism was associated with ARDS in two cohorts of at-risk hospitalized adults. Although age-related effect modification was observed only in the prospective biomarker cohort, the EHR cohort identified a consistent association between MUC5B and ARDS risk regardless of age and a novel association with oxygenation impairment. Our study highlights the potential for EHR biobanks to enable precision-medicine ARDS studies.
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