Effects of obesogenic diet and 17β-estradiol in female mice with APOE 3/3, 3/4, and 4/4 genotypes

IF 4.1 2区医学 Q2 GERIATRICS & GERONTOLOGY

Frontiers in Aging Neuroscience Pub Date : 2024-09-13 DOI:10.3389/fnagi.2024.1415072

Amy Christensen, Cassandra J. McGill, Wenjie Qian, Christian J. Pike

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引用次数: 0

Abstract

The main genetic risk factor for Alzheimer’s disease (AD) is the apolipoprotein E ε4 allele (APOE4). AD risk associated with APOE4 disproportionately affects women. Furthermore, human and rodent studies indicate that the cognitive deficits associated with APOE4 are greater in females. One modifiable AD risk factor is obesity during middle age. Given that approximately two-thirds of US adults are overweight, it is important to understand how obesity affects AD risk, how it interacts with APOE4, and the extent to which its detrimental effects can be mitigated with therapeutics. One intervention study for women is estrogen-based hormone therapy, which can exert numerous health benefits when administered in early middle age. No experimental studies have examined the interactions among APOE4, obesity, and hormone therapy in aging females. To begin to explore these issues, we considered how obesity outcomes are affected by treatment with estradiol at the onset of middle age in female mice with human APOE3 and APOE4. Furthermore, to explore how gene dosage affects outcomes, we compared mice homozygous for APOE3 (3/3) and homozygous (4/4) or hemizygous (3/4) for APOE4. Mice were examined over a 4-month period that spans the transition into reproductive senescence, a normal age-related change that models many aspects of human perimenopause. Beginning at 5 months of age, mice were maintained on a control diet (10% fat) or high-fat diet (HFD; 60% fat). After 8 weeks, by which time obesity was present in all HFD groups, mice were implanted with an estradiol or vehicle capsule that was maintained for the final 8 weeks. Animals were assessed on a range of metabolic and neural measures. Overall, APOE4 was associated with poorer metabolic function and cognitive performance. However, an obesogenic diet induced relatively greater impairments in metabolic function and cognitive performance in APOE3/3 mice. Estradiol treatment improved metabolic and cognitive outcomes across all HFD groups, with APOE4/4 generally exhibiting the greatest benefit. APOE3/4 mice were intermediate to the homozygous genotypes on many measures but also exhibited unique profiles. Together, these findings highlight the importance of the APOE genotype as a modulator of the risks associated with obesity and the beneficial outcomes of estradiol.

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肥胖饮食和 17β-estradiol 对 APOE 3/3、3/4 和 4/4 基因型雌性小鼠的影响

阿尔茨海默病（AD）的主要遗传风险因素是载脂蛋白 E ε4等位基因（APOE4）。与 APOE4 相关的阿兹海默症风险对女性的影响尤为严重。此外，人类和啮齿类动物研究表明，与 APOE4 相关的认知缺陷在女性中更为严重。中年肥胖是一个可改变的痴呆症风险因素。鉴于大约三分之二的美国成年人超重，了解肥胖如何影响注意力缺失症风险、肥胖如何与 APOE4 相互影响以及肥胖的不利影响在多大程度上可以通过治疗得到缓解就显得尤为重要。针对女性的一项干预研究是基于雌激素的荷尔蒙疗法，这种疗法在中年早期施用可为健康带来诸多益处。目前还没有实验研究对老年女性的 APOE4、肥胖和激素疗法之间的相互作用进行研究。为了开始探索这些问题，我们考虑了在人类 APOE3 和 APOE4 的雌性小鼠中，在中年开始时使用雌二醇治疗对肥胖结果的影响。此外，为了探索基因剂量如何影响结果，我们比较了 APOE3（3/3）同基因小鼠和 APOE4 同基因小鼠（4/4）或半同基因小鼠（3/4）。对小鼠进行了为期 4 个月的检查，这段时间跨越了生殖衰老期，这是一种与年龄相关的正常变化，在许多方面模拟了人类的围绝经期。小鼠从 5 个月大开始，以对照组饮食（10% 脂肪）或高脂饮食（HFD；60% 脂肪）饲养。8 周后，即所有高脂饮食组都出现肥胖时，给小鼠植入雌二醇或载体胶囊，并维持 8 周。对动物进行了一系列代谢和神经方面的评估。总体而言，APOE4 与代谢功能和认知能力较差有关。然而，肥胖饮食对 APOE3/3 小鼠代谢功能和认知能力的损害相对更大。雌二醇治疗可改善所有高密度脂蛋白膳食组的代谢和认知结果，APOE4/4组的获益最大。APOE3/4小鼠在许多指标上介于同型基因型之间，但也表现出独特的特征。总之，这些发现凸显了 APOE 基因型作为肥胖相关风险和雌二醇有益结果调节器的重要性。

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来源期刊

Frontiers in Aging Neuroscience GERIATRICS & GERONTOLOGY-NEUROSCIENCES

CiteScore

6.30

自引率

8.30%

发文量

1426

期刊介绍： Frontiers in Aging Neuroscience is a leading journal in its field, publishing rigorously peer-reviewed research that advances our understanding of the mechanisms of Central Nervous System aging and age-related neural diseases. Specialty Chief Editor Thomas Wisniewski at the New York University School of Medicine is supported by an outstanding Editorial Board of international researchers. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide.