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首页> 外文期刊>Psychoneuroendocrinology: An International Journal >Polygenic risk for circulating reproductive hormone levels and their influence on hippocampal volume and depression susceptibility
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Polygenic risk for circulating reproductive hormone levels and their influence on hippocampal volume and depression susceptibility

机译:循环生殖激素水平的多基因风险及其对海马体积和抑郁症易感性的影响

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Altered reproductive hormone levels have been associated with the pathophysiology of depressive disorders and this risk may be imparted by their modulatory effect upon hippocampal structure and function. Currently it is unclear whether altered levels of reproductive hormones are causally associated with hippocampal volume reductions and the risk of depressive disorders. Here, we utilize genome-wide association study (GWAS) summary statistics from a GWAS focusing on reproductive hormones, consisting of 2913 individuals. Using this data, we generated polygenic risk scores (PRS) for estradiol, progesterone, prolactin and testosterone in the European RADIANT cohort consisting of 176 postpartum depression (PPD) cases (100% female, mean age: 41.6 years old), 2772 major depressive disorder (MDD) cases (68.6% female, mean age: 46.9 years old) and 1588 control participants (62.5% female, mean age: 42.4 years old), for which there was also a neuroimaging subset of 111 individuals (60.4% female, mean age: 50.0 years old). Only the best-fit PRS for estradiol showed a significant negative association with hippocampal volume, as well as many of its individual subfields; including the molecular layer and granule cell layer of the dentate gyrus, subiculum, CA1, CA2/3 and CA4 regions. Interestingly, several of these subfields are implicated in adult hippocampal neurogenesis. When we tested the same estradiol PRS for association with case-control status for PPD or MDD there was no significant relationship observed. Here, we provide evidence that genetic risk for higher plasma estradiol is negatively associated with hippocampal volume, but this does not translate into an increased risk of MDD or PPD. This work suggests that the relationship between reproductive hormones, the hippocampus, and depression is complex, and that there may not be a clear-cut pathway for etiology or risk moderation.
机译:改变的生殖激素水平与抑郁症的病理生理学有关,并且可以通过对海马结构和功能的调节作用来赋予这种风险。目前目前还不清楚生殖激素的改变水平是否因海马体积还原和抑郁症的风险而导致局部相关。在这里,我们利用基因组关联研究(GWAS)概述统计从聚集在生殖激素上的GWAS,由2913个人组成。使用这种数据,我们为欧洲辐射队列中的雌二醇,黄体酮,催乳素和睾酮产生的多基因风险评分(PRS)组成(PPD)病例(100%女性,意思年龄:41.6岁),2772个主要抑郁症疾病(MDD)病例(女性,意思年龄:46.9岁)和1588名控制参与者(62.5%的女性,意思年龄:42.4岁),也有111个个体的神经影像集团(60.4%的女性,意思是年龄:50.0岁)。只有雌二醇的最佳拟合PRS显示出与海马体积的显着阴性关联,以及其各个子场的许多;包括牙齿转酯,亚细胞,Ca1,Ca2 / 3和Ca4区的分子层和颗粒细胞层。有趣的是,这些子场中的几个涉及成年海马神经发生。当我们测试与PPD或MDD的案例控制状态相关联的雌二醇PR时,没有观察到具有重要关系。在这里,我们提供了较高血浆雌二醇的遗传风险与海马体积产生的遗传风险,但这并未转化为MDD或PPD的风险增加。这项工作表明,生殖激素,海马和抑郁症之间的关系是复杂的,并且由于病因或风险适度可能没有明确的途径。

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