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核受体和膜结合孕激素受体在女性生殖道中的推测作用。

The putative roles of nuclear and membrane-bound progesterone receptors in the female reproductive tract.

机构信息

Institute of Animal Reproduction and Food Research, Polish Academy of Sciences, Tuwima 10, 10-748 Olsztyn, Poland.

出版信息

Reprod Biol. 2013 Dec;13(4):279-89. doi: 10.1016/j.repbio.2013.09.001. Epub 2013 Sep 14.

Abstract

Progesterone produced by the corpus luteum (CL) is a key regulator of normal cyclical reproductive functions in the females of mammalian species. The physiological effects of progesterone are mediated by the canonical genomic pathway after binding of progesterone to its specific nuclear progesterone receptor (PGR), which acts as a ligand-activated transcription factor and has two main isoforms, PGRA and PGRB. These PGR isoforms play different roles in the cell; PGRB acts as an activator of progesterone-responsive genes, while PGRA can inhibit the activity of PGRB. The ratio of these isoforms changes during the estrous cycle and pregnancy, and it corresponds to the different levels of progesterone signaling occurring in the reproductive tract. Progesterone exerts its effects on cells also by a non-genomic mechanism by the interaction with the progesterone-binding membrane proteins including the progesterone membrane component (PGRMC) 1 and 2, and the membrane progestin receptors (mPRs). These receptors rapidly activate the appropriate intracellular signal transduction pathways, and subsequently they can initiate specific cell responses or modulate genomic cell responses. The diversity of progesterone receptors and their cellular actions enhances the role of progesterone as a factor regulating the function of the reproductive system and other organs. This paper deals with the possible involvement of nuclear and membrane-bound progesterone receptors in the function of target cells within the female reproductive tract.

摘要

黄体(CL)产生的孕激素是调节哺乳动物雌性正常周期性生殖功能的关键调节剂。孕激素的生理作用是通过孕激素与其特异性核孕激素受体(PGR)结合后的经典基因组途径介导的,PGR 作为配体激活转录因子,有两种主要的同工型,PGRA 和 PGRB。这些 PGR 同工型在细胞中发挥不同的作用;PGRB 作为孕激素反应基因的激活剂,而 PGRA 可以抑制 PGRB 的活性。这些同工型的比例在发情周期和妊娠期间发生变化,与生殖道中发生的不同水平的孕激素信号相对应。孕激素还通过与包括孕激素膜成分(PGRMC)1 和 2 以及膜孕激素受体(mPR)在内的孕激素结合膜蛋白的非基因组机制发挥作用。这些受体可快速激活适当的细胞内信号转导途径,随后可引发特定的细胞反应或调节基因组细胞反应。孕激素受体的多样性及其细胞作用增强了孕激素作为调节生殖系统和其他器官功能的因素的作用。本文探讨了核孕激素受体和膜结合孕激素受体在雌性生殖道靶细胞功能中的可能参与。

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