绝经后妇女的 APOE、2 型糖尿病和心血管疾病之间的关系。

Michelle M Dunk, Ira Driscoll, Mark A Espeland, Kathleen M Hayden, Simin Liu, Rami Nassir, Ginny Natale, Aladdin H Shadyab, Jo Ann E Manson
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引用次数: 0

摘要

背景:载脂蛋白E(APOE)ε4等位基因、2型糖尿病(T2DM)和心血管疾病(CVD)是公认的痴呆症风险因素。APOE与T2DM和心血管疾病发病率之间的关系尚不完全清楚,但可能揭示痴呆症发病机制:方法:研究人员纳入了来自妇女健康倡议激素疗法临床试验的绝经后妇女(N=6795),这些妇女进行了 APOE 基因分型,且之前未诊断出 T2DM 或心血管疾病。我们使用 Cox 回归法研究了 APOE 状态(APOE2+ [ε2/ε2、ε2/ε3]、APOE3 [ε3/ε3]和 APOE4+ [ε4/ε4、ε3/ε4] 携带者)与 T2DM、冠心病 (CHD)、中风和总心血管疾病事件发生率的关系。对基线非他汀类药物使用者的心血管疾病结果进行了研究,并根据随访期间他汀类药物的使用情况进行了调整,以考虑他汀类药物可能造成的混杂因素:在所有参与者(平均年龄为 66.7±6.5 岁,100% 为非西班牙裔白人)中,有 451 人(6.6%)在基线时使用他汀类药物。在随访期间(T2DM 和心血管疾病的平均随访时间分别为 14.9 年和 16.0 年),分别有 1,564 人和 1,578 人罹患 T2DM 和心血管疾病。T2DM发病率与APOE状态无显著差异(ps≥0.09)。在非他汀类药物使用者中,与 APOE3 携带者相比,APOE4+ 的总心血管疾病发病率更高(危险比 [95% 置信区间]=1.18 [1.02-1.38],P=0.03),但单独研究时,冠心病(1.09 [0.87-1.36],P=0.47)和中风(1.14 [0.91-1.44],P=0.27)的风险并无显著升高。APOE2+和APOE3携带者之间的心血管疾病结果没有差异(ps≥0.11):结论:绝经后妇女的 T2DM 风险在 APOE 状态上没有差异,但未使用他汀类药物的 APOE4+ 携带者发生总心血管疾病事件的风险增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Relationships between APOE, Type 2 Diabetes, and Cardiovascular Disease in Postmenopausal Women.

Background: The Apolipoprotein E (APOE) ε4 allele, type 2 diabetes mellitus (T2DM), and cardiovascular disease (CVD) are well-established risk factors for dementia. Relationships between APOE and incidence of T2DM and CVD are not fully understood but may shed light on the mechanisms underlying dementia pathogenesis.

Methods: Postmenopausal women (N=6,795) from the Women's Health Initiative hormone therapy clinical trial with APOE genotyping and no prior diagnosis of T2DM or CVD were included. We examined associations of APOE status (APOE2+ [ε2/ε2, ε2/ε3], APOE3 [ε3/ε3], and APOE4+ [ε4/ε4, ε3/ε4] carriers) with incidence of T2DM, coronary heart disease (CHD), stroke, and total CVD events using Cox regression. CVD outcomes were examined in baseline non-statin users and adjusted for statin initiation over follow-up to account for possible confounding by statins.

Results: Among all participants (mean age 66.7±6.5 years, 100% non-Hispanic white), 451 (6.6%) were using statins at baseline. Over the follow-up (mean 14.9 and 16.0 years for T2DM and CVD, respectively), 1,564 participants developed T2DM and 1,578 developed CVD. T2DM incidence did not differ significantly by APOE status (ps≥0.09). Among non-statin users, APOE4+ had higher incidence of total CVD (hazard ratio [95% confidence interval]=1.18 [1.02-1.38], p=0.03) compared to APOE3 carriers, but risks for CHD (1.09 [0.87-1.36], p=0.47) and stroke (1.14 [0.91-1.44], p=0.27) were not significantly elevated when examined individually. CVD outcomes did not differ between APOE2+ and APOE3 carriers (ps≥0.11).

Conclusions: T2DM risk did not differ by APOE status among postmenopausal women, but APOE4+ carriers not using statins had an increased risk of total CVD events.

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