促性腺激素水平升高与中年女性罹患阿尔茨海默病的生物标志物风险增加有关

Matilde Nerattini, Federica Rubino, Steven Jett, Caroline Andy, Camila Boneu, Camila Zarate, Caroline Carlton, Susan Loeb-Zeitlin, Y. Havryliuk, S. Pahlajani, Schantel Williams, Valentina Berti, Paul Christos, Matthew Fink, Jonathan P. Dyke, R. Brinton, Lisa Mosconi
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引用次数: 0

摘要

在临床前研究中,垂体促性腺激素、卵泡刺激素(FSH)和黄体生成素(LH)的绝经期升高会引发雌性动物阿尔茨海默病(AD)的病理变化和突触丧失。我们对 191 名 40-65 岁的女性进行了研究,其中包括 45 名绝经前女性、67 名围绝经期女性和 79 名绝经后女性,她们都具有晚发阿兹海默症的风险因素,并接受了临床、实验室、认知检查和容积核磁共振成像扫描。其中一半人完成了 11C 匹兹堡化合物 B(PiB)淀粉样蛋白-β(Aβ)PET 扫描。采用基于体素的分析方法研究了血清FSH、LH和生物标记物之间的关系,包括总体关系和绝经状态分层关系。FSH水平与额叶皮层的Aβ负荷呈正相关(多变量调整后P≤0.05,经家系智型误差校正,FWE),这一效应由绝经后组驱动(多变量调整后PFWE≤0.044)。LH 水平也与额叶皮层的 Aβ 负荷有关,但没有经过多变量调整。FSH和LH与额叶皮层灰质体积(GMV)呈负相关(总体和各绝经组)(多变量调整后PFWE≤0.040),FSH与ROI海马体积略有关联(多变量调整后P = 0.058)。这些关联与年龄、临床混杂因素、绝经类型、激素治疗状态、抑郁症病史、APOE-4 状态和雌二醇的区域效应无关。血清促性腺激素水平(尤其是 FSH)的升高与中年女性面临 AD 风险的某些 AD 易感区域的 Aβ 负荷升高和 GMV 降低有关。这些发现与临床前研究结果一致,为降低AD风险的精准医疗策略提供了探索性激素靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Elevated gonadotropin levels are associated with increased biomarker risk of Alzheimer's disease in midlife women
In preclinical studies, menopausal elevations in pituitary gonadotropins, follicle-stimulating hormone (FSH) and luteinizing hormone (LH), trigger Alzheimer's disease (AD) pathology and synaptic loss in female animals. Herein, we took a translational approach to test whether gonadotropin elevations are linked to AD pathophysiology in women.We examined 191 women ages 40–65 years, carrying risk factors for late-onset AD, including 45 premenopausal, 67 perimenopausal, and 79 postmenopausal participants with clinical, laboratory, cognitive exams, and volumetric MRI scans. Half of the cohort completed 11C-Pittsburgh Compound B (PiB) amyloid-β (Aβ) PET scans. Associations between serum FSH, LH and biomarkers were examined using voxel-based analysis, overall and stratified by menopause status. Associations with region-of-interest (ROI) hippocampal volume, plasma estradiol levels, APOE-4 status, and cognition were assessed in sensitivity analyses.FSH levels were positively associated with Aβ load in frontal cortex (multivariable adjusted P ≤ 0.05, corrected for family wise type error, FWE), an effect that was driven by the postmenopausal group (multivariable adjusted PFWE ≤ 0.044). LH levels were also associated with Aβ load in frontal cortex, which did not survive multivariable adjustment. FSH and LH were negatively associated with gray matter volume (GMV) in frontal cortex, overall and in each menopausal group (multivariable adjusted PFWE ≤ 0.040), and FSH was marginally associated with ROI hippocampal volume (multivariable adjusted P = 0.058). Associations were independent of age, clinical confounders, menopause type, hormone therapy status, history of depression, APOE-4 status, and regional effects of estradiol. There were no significant associations with cognitive scores.Increasing serum gonadotropin levels, especially FSH, are associated with higher Aβ load and lower GMV in some AD-vulnerable regions of midlife women at risk for AD. These findings are consistent with preclinical work and provide exploratory hormonal targets for precision medicine strategies for AD risk reduction.
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