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孕激素抑制子宫内膜中催产素信号。

Progesterone inhibition of oxytocin signaling in endometrium.

机构信息

Division of Reproductive and Developmental Sciences, Oregon National Primate Research Center, Oregon Health & Science University Beaverton, OR, USA.

出版信息

Front Neurosci. 2013 Aug 7;7:138. doi: 10.3389/fnins.2013.00138. eCollection 2013.

Abstract

Expression of the oxytocin receptor (OXTR) in the endometrium of ruminant species is regulated by the ovarian steroids progesterone (P) and estradiol (E). Near the end of the estrous cycle, long-term exposure of endometrial epithelial cells to P results in loss of genomic P receptors (PGRs), leading to an increase in E receptors (ERs). Genomic regulation of the OXTR is mediated via suppression of ER signaling by P. Upon OT binding at the plasma membrane of endometrial cells, a signaling cascade is generated stimulating release of prostaglandin F2α (PGF2α). Transport of PGF2α to the ovary results in release of OT by luteal cells in a positive feedback loop leading to luteal regression. This signaling cascade can be rapidly blocked by exposing endometrial cells to physiologic levels of P. This mini review will focus on the mechanisms by which P may act to block OXTR signaling and the luteolytic cascade in the ruminant endometrium, with special focus on both non-genomic signaling pathways and non-receptor actions of P at the level of the plasma membrane. While this review focuses on ruminant species, non-classical blockage of OXTR signaling may be important for fertility in women.

摘要

在反刍动物物种的子宫内膜中,催产素受体 (OXTR) 的表达受卵巢类固醇孕酮 (P) 和雌二醇 (E) 的调节。在发情周期接近尾声时,子宫内膜上皮细胞长期暴露于 P 会导致基因组 P 受体 (PGRs) 的丧失,从而导致 E 受体 (ERs) 的增加。OXTR 的基因组调节是通过 P 抑制 ER 信号传导来介导的。在 OT 与子宫内膜细胞的质膜结合后,会产生一个信号级联反应,刺激前列腺素 F2α (PGF2α) 的释放。PGF2α 向卵巢的转运导致黄体细胞释放 OT,形成正反馈循环,导致黄体退化。这种信号级联可以通过将子宫内膜细胞暴露于生理水平的 P 来迅速阻断。这篇综述将重点讨论 P 可能作用于阻断反刍动物子宫内膜中 OXTR 信号和溶黄体级联的机制,特别关注 P 在质膜水平的非基因组信号通路和非受体作用。虽然本综述重点关注反刍动物物种,但 OXTR 信号的非经典阻断对于女性的生育能力可能很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c921/3735988/a97f34e25bb6/fnins-07-00138-g0001.jpg

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