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新型雌激素受体β激动剂EGX358与基因型对阿尔茨海默病小鼠模型的记忆、血管舒缩及焦虑结果产生影响。

The novel estrogen receptor beta agonist EGX358 and genotype influence memory, vasomotor, and anxiety outcomes in an Alzheimer's mouse model.

作者信息

Schwabe M R, Fleischer A W, Kuehn R K, Chaudhury S, York J M, Sem D S, Donaldson W A, LaDu M J, Frick K M

机构信息

Department of Psychology, University of Wisconsin-Milwaukee, Milwaukee, WI, United States.

Department of Chemistry, Marquette University, Milwaukee, WI, United States.

出版信息

Front Aging Neurosci. 2024 Nov 13;16:1477045. doi: 10.3389/fnagi.2024.1477045. eCollection 2024.

Abstract

INTRODUCTION

Alzheimer's disease (AD) prevalence and severity are associated with increased age, female sex, and apolipoprotein E4 (APOE4) genotype. Although estrogen therapy (ET) effectively reduces symptoms of menopause including hot flashes and anxiety, and can reduce dementia risk, it is associated with increased risks of breast and uterine cancer due to estrogen receptor alpha (ERα)-mediated increases in cancer cell proliferation. Because ERβ activation reduces this cell proliferation, selective targeting of ERβ may provide a safer method of improving memory and reducing hot flashes in menopausal women, including those with AD. APOE genotype influences the response to ET, although it is unknown whether effects of ERβ activation vary by genotype.

METHODS

Here, we tested the ability of long-term oral treatment with a novel highly selective ERβ agonist, EGX358, to enhance object recognition and spatial recognition memory, reduce drug-induced hot flashes, and influence anxiety-like behaviors in female mice expressing 5 familial AD mutations (5xFAD-Tg) and human APOE3 (E3FAD) or APOE3 and APOE4 (E3/4FAD). Mice were ovariectomized at 5 months of age and were then treated orally with vehicle (DMSO) or EGX358 (10 mg/kg/day) via hydrogel for 8 weeks. Spatial and object recognition memory were tested in object placement (OP) and object recognition (OR) tasks, respectively, and anxiety-like behaviors were tested in the open field (OF) and elevated plus maze (EPM). Hot flash-like symptoms (change in tail skin temperature) were measured following injection of the neurokinin receptor agonist senktide (0.5 mg/kg).

RESULTS

EGX358 enhanced object recognition memory in E3FAD and E3/4FAD mice but did not affect spatial recognition memory. EGX358 also reduced senktide-induced tail temperature elevations in E3FAD, but not E3/4FAD, females. EGX358 did not influence anxiety-like behaviors or body weight.

DISCUSSION

These data indicate that highly selective ERβ agonism can facilitate object recognition memory in both APOE3 homozygotes and APOE3/4 heterozygotes, but only reduce the magnitude of a drug-induced hot flash in APOE3 homozygotes, suggesting that APOE4 genotype may blunt the beneficial effects of ET on hot flashes. Collectively, these data suggest a potentially beneficial effect of selective ERβ agonism for memory and hot flashes in females with AD-like pathology, but that APOE genotype plays an important role in responsiveness.

摘要

引言

阿尔茨海默病(AD)的患病率和严重程度与年龄增长、女性性别以及载脂蛋白E4(APOE4)基因型相关。尽管雌激素疗法(ET)能有效减轻更年期症状,包括潮热和焦虑,且可降低痴呆风险,但由于雌激素受体α(ERα)介导癌细胞增殖增加,该疗法会增加患乳腺癌和子宫癌的风险。因为ERβ激活可减少这种细胞增殖,所以选择性靶向ERβ可能为改善绝经后女性(包括患有AD的女性)的记忆力和减轻潮热提供一种更安全的方法。APOE基因型会影响对ET的反应,不过ERβ激活的效果是否因基因型而异尚不清楚。

方法

在此,我们测试了新型高选择性ERβ激动剂EGX358长期口服治疗对表达5种家族性AD突变(5xFAD-Tg)以及人类APOE3(E3FAD)或APOE3和APOE4(E3/4FAD)的雌性小鼠的物体识别和空间识别记忆的增强能力、对药物诱导的潮热的减轻作用以及对焦虑样行为的影响。小鼠在5月龄时进行卵巢切除术,然后通过水凝胶口服给予溶剂(二甲基亚砜)或EGX358(10毫克/千克/天),持续8周。分别在物体放置(OP)任务和物体识别(OR)任务中测试空间和物体识别记忆,并在旷场(OF)和高架十字迷宫(EPM)中测试焦虑样行为。在注射神经激肽受体激动剂森克肽(0.5毫克/千克)后测量潮热样症状(尾部皮肤温度变化)。

结果

EGX358增强了E3FAD和E3/4FAD小鼠的物体识别记忆,但不影响空间识别记忆。EGX358还降低了E3FAD雌性小鼠中森克肽诱导的尾部温度升高,但对E3/4FAD雌性小鼠没有影响。EGX358不影响焦虑样行为或体重。

讨论

这些数据表明,高选择性ERβ激动作用可促进APOE3纯合子和APOE3/4杂合子的物体识别记忆,但仅能降低APOE3纯合子中药物诱导的潮热程度,这表明APOE4基因型可能会削弱ET对潮热的有益作用。总体而言,这些数据表明选择性ERβ激动作用对具有AD样病理的女性的记忆和潮热可能具有潜在的有益影响,但APOE基因型在反应性方面起着重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6383/11613887/8a7d6f1ae316/fnagi-16-1477045-g001.jpg

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