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APOE 基因对心血管疾病和癌症发病年龄的影响在不同年龄、性别和人类世代之间的权衡。

Trade-off in the effect of the APOE gene on the ages at onset of cardiocascular disease and cancer across ages, gender, and human generations.

机构信息

Center for Population Health and Aging, Duke University, Durham, North Carolina 27708, USA.

出版信息

Rejuvenation Res. 2013 Feb;16(1):28-34. doi: 10.1089/rej.2012.1362.

Abstract

Decades of studies of candidate genes show their complex role in aging-related traits. We focus on apolipoprotein E e2/3/4 polymorphism and ages at onset of cardiovascular diseases (CVD) and cancer in the parental and offspring generations of the Framingham Heart Study participants to gain insights on the role of age and gender across generations in genetic trade-offs. The analyses show that the apolipoprotein E e4 allele carriers live longer lives without cancer than the non-e4 allele carriers in each generation. The role of the e4 allele in onset of CVD is age- and generation-specific, constituting two modes of sexually dimorphic genetic trade-offs. In offspring, the e4 allele confers risk of CVD primarily in women and can protect against cancer primarily in men of the same age. In the parental generation, genetic trade-off is seen in different age groups, with a protective role of the e4 allele against cancer in older men and its detrimental role in CVD in younger women. The puzzling complexity of genetic mechanisms working in different genders, ages, and environments calls for more detail and systemic analyses beyond those adapted in current large-scale genetic association studies.

摘要

几十年来,对候选基因的研究表明它们在与衰老相关的特征中起着复杂的作用。我们专注于载脂蛋白 E e2/3/4 多态性以及弗雷明汉心脏研究参与者的父母和后代几代人中心血管疾病 (CVD) 和癌症的发病年龄,以深入了解代际之间年龄和性别在遗传权衡中的作用。分析表明,在每一代中,载脂蛋白 E e4 等位基因携带者的无癌寿命比非 e4 等位基因携带者长。e4 等位基因在 CVD 发病中的作用具有年龄和世代特异性,构成了两种性别二态遗传权衡模式。在后代中,e4 等位基因主要在女性中赋予 CVD 风险,并且可以主要在同一年龄的男性中预防癌症。在父母一代中,遗传权衡出现在不同的年龄组中,e4 等位基因对老年男性的癌症具有保护作用,对年轻女性的 CVD 具有不利作用。在不同性别、年龄和环境中发挥作用的遗传机制的复杂令人费解,需要超越当前大规模遗传关联研究中采用的更详细和系统的分析。

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