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胎儿雄激素暴露是成年男性代谢健康的决定因素。

Fetal androgen exposure is a determinant of adult male metabolic health.

机构信息

School of Applied Science, Edinburgh Napier University, Edinburgh, EH11 4BN, UK.

Institute of Medical Sciences, School of Medicine, Medical Sciences & Nutrition, University of Aberdeen, Aberdeen, AB25 2ZD, UK.

出版信息

Sci Rep. 2019 Dec 27;9(1):20195. doi: 10.1038/s41598-019-56790-4.

Abstract

Androgen signalling is a critical driver of male development. Fetal steroid signalling can be dysregulated by a range of environmental insults and clinical conditions. We hypothesised that poor adult male health was partially attributable to aberrant androgen exposure during development. Testosterone was directly administered to developing male ovine fetuses to model excess prenatal androgenic overexposure associated with conditions such as polycystic ovary syndrome (PCOS). Such in utero androgen excess recreated the dyslipidaemia and hormonal profile observed in sons of PCOS patients. 1,084 of 15,134 and 408 of 2,766 quantifiable genes and proteins respectively, were altered in the liver during adolescence, attributable to fetal androgen excess. Furthermore, prenatal androgen excess predisposed to adolescent development of an intrahepatic cholestasis-like condition with attendant hypercholesterolaemia and an emergent pro-fibrotic, pro-oxidative stress gene and protein expression profile evident in both liver and circulation. We conclude that prenatal androgen excess is a previously unrecognised determinant of lifelong male metabolic health.

摘要

雄激素信号是男性发育的关键驱动因素。胎儿类固醇信号可能会受到多种环境损伤和临床情况的失调。我们假设,男性成年后健康状况不佳部分归因于发育过程中雄激素暴露异常。我们向发育中的雄性绵羊胎儿直接给予睾酮,以模拟与多囊卵巢综合征(PCOS)等疾病相关的产前雄激素过度暴露。这种宫内雄激素过多会重现 PCOS 患者儿子中观察到的血脂异常和激素谱。在青春期期间,肝脏中分别有 1084 个和 408 个可量化的基因和蛋白质发生了改变,这归因于胎儿雄激素过多。此外,产前雄激素过多易导致青少年时期出现类似于肝内胆汁淤积的情况,伴有胆固醇升高,以及在肝脏和循环中均出现明显的促纤维化、促氧化应激基因和蛋白质表达谱。我们的结论是,产前雄激素过多是男性终生代谢健康的一个以前未被认识到的决定因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6e5/6934666/6208346cedc1/41598_2019_56790_Fig1_HTML.jpg

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