Heart Failure Risk Among African-American Women With an ICAM1 Missense Variant

IF 10.3 1区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
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Abstract

Background

A common genetic variant of ICAM1 among African-American individuals (rs5491; p.K56M) is associated with heart failure (HF) hospitalization, but whether this risk is specific to heart failure with preserved ejection fraction (HFpEF) remains unclear. Older women are at high risk for HFpEF, and the relationship between rs5491 and HFpEF across the age spectrum is unknown.

Objectives

This study assessed risk of HF and its subtypes conferred by ICAM1 p.K56M (rs5491).

Methods

Associations of rs5491 with risk of HF and its subtypes were estimated among African American individuals in WHI (Women’s Health Initiative). The study evaluated whether the association between rs5491 and HF hospitalizations was modified by baseline age. Subsequently, African-American women in WHI and MESA (Multi-Ethnic Study of Atherosclerosis) were pooled and analyses were repeated.

Results

Among 8,401 women in WHI, the minor allele frequency of rs5491 was 20.7%, and 731 HF hospitalizations occurred over 19.2 years. The rs5491 variant was not associated with HF or its subtypes across WHI. Interaction analyses suggested that age as a continuous variable modified the association of rs5491 with HFpEF hospitalization (interaction P = 0.04). Upon categorizing women into age decades, rs5491 conferred increased risk of HFpEF among women ≥70 years (HR per additional rs5491 allele: 1.82 [95% CI: 1.25-2.65]; P = 0.002) but was not associated with HFpEF risk among women <70 years. Pooling African-American women in WHI (n = 8,401) and MESA (n = 856) demonstrated that the effect modification by age on the association of rs5491 with HFpEF became more significant (interaction P = 0.009), with consistent HFpEF risk effect estimates among women ≥70 years.

Conclusions

ICAM1 p.K56M (rs5491) is associated with HFpEF among African-American women ≥70 years.

患有 ICAM1 缺义变异的非裔美国妇女患心力衰竭的风险
背景:非裔美国人中一种常见的 ICAM1 遗传变异(rs5491; p.K56M)与心力衰竭(HF)住院治疗有关,但这种风险是否专属于射血分数保留型心力衰竭(HFpEF)仍不清楚。老年女性是 HFpEF 的高危人群,而 rs5491 与 HFpEF 在不同年龄段的关系尚不清楚:本研究评估了 ICAM1 p.K56M (rs5491) 带来的高房颤风险及其亚型:方法:在WHI(妇女健康倡议)的非裔美国人中估算了rs5491与心房颤动风险及其亚型的相关性。该研究评估了 rs5491 与心房颤动住院之间的关系是否会因基线年龄而改变。随后,对WHI和MESA(多种族动脉粥样硬化研究)中的非裔美国妇女进行了汇总,并重复进行了分析:在 8,401 名参加 WHI 的女性中,rs5491 的小等位基因频率为 20.7%,在 19.2 年中有 731 人因高血压住院治疗。在整个 WHI 中,rs5491 变体与心房颤动或其亚型无关。交互分析表明,作为连续变量的年龄改变了 rs5491 与 HFpEF 住院的相关性(交互 P = 0.04)。将妇女分为不同年龄段后,rs5491 会增加≥70 岁妇女的 HFpEF 风险(每增加一个 rs5491 等位基因的 HR:1.82 [95% CI:1.25-2.65];P = 0.002),但与妇女的 HFpEF 风险无关:ICAM1 p.K56M (rs5491) 与年龄≥70 岁的非裔美国妇女的 HFpEF 相关。
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来源期刊
JACC. Heart failure
JACC. Heart failure CARDIAC & CARDIOVASCULAR SYSTEMS-
CiteScore
21.20
自引率
2.30%
发文量
164
期刊介绍: JACC: Heart Failure publishes crucial findings on the pathophysiology, diagnosis, treatment, and care of heart failure patients. The goal is to enhance understanding through timely scientific communication on disease, clinical trials, outcomes, and therapeutic advances. The Journal fosters interdisciplinary connections with neuroscience, pulmonary medicine, nephrology, electrophysiology, and surgery related to heart failure. It also covers articles on pharmacogenetics, biomarkers, and metabolomics.
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