Brinton Roberta Diaz, Thompson Richard F, Foy Michael R, Baudry Michel, Wang Junming, Finch Caleb E, Morgan Todd E, Pike Christian J, Mack Wendy J, Stanczyk Frank Z, Nilsen Jon
Department of Pharmacology and Pharmaceutical Sciences, University of Southern California, School of Pharmacy, 1985 Zonal Avenue, Los Angeles, CA 90089, USA.
Front Neuroendocrinol. 2008 May;29(2):313-39. doi: 10.1016/j.yfrne.2008.02.001. Epub 2008 Feb 23.
Emerging data indicate that progesterone has multiple non-reproductive functions in the central nervous system to regulate cognition, mood, inflammation, mitochondrial function, neurogenesis and regeneration, myelination and recovery from traumatic brain injury. Progesterone-regulated neural responses are mediated by an array of progesterone receptors (PR) that include the classic nuclear PRA and PRB receptors and splice variants of each, the seven transmembrane domain 7TMPRbeta and the membrane-associated 25-Dx PR (PGRMC1). These PRs induce classic regulation of gene expression while also transducing signaling cascades that originate at the cell membrane and ultimately activate transcription factors. Remarkably, PRs are broadly expressed throughout the brain and can be detected in every neural cell type. The distribution of PRs beyond hypothalamic borders, suggests a much broader role of progesterone in regulating neural function. Despite the large body of evidence regarding progesterone regulation of reproductive behaviors and estrogen-inducible responses as well as effects of progesterone metabolite neurosteroids, much remains to be discovered regarding the functional outcomes resulting from activation of the complex array of PRs in brain by gonadally and/or glial derived progesterone. Moreover, the impact of clinically used progestogens and developing selective PR modulators for targeted outcomes in brain is a critical avenue of investigation as the non-reproductive functions of PRs have far-reaching implications for hormone therapy to maintain neurological health and function throughout menopausal aging.
新出现的数据表明,孕酮在中枢神经系统具有多种非生殖功能,可调节认知、情绪、炎症、线粒体功能、神经发生与再生、髓鞘形成以及创伤性脑损伤后的恢复。孕酮调节的神经反应由一系列孕酮受体(PR)介导,这些受体包括经典的核PRA和PRB受体及其各自的剪接变体、七跨膜结构域7TMPRβ和膜相关的25-Dx PR(PGRMC1)。这些PR可诱导基因表达的经典调节,同时也转导起源于细胞膜并最终激活转录因子的信号级联反应。值得注意的是,PR在整个大脑中广泛表达,并且可以在每种神经细胞类型中检测到。PR在下丘脑边界之外的分布表明孕酮在调节神经功能方面具有更广泛的作用。尽管有大量关于孕酮对生殖行为的调节、雌激素诱导反应以及孕酮代谢物神经甾体的作用的证据,但关于性腺和/或胶质细胞衍生的孕酮激活大脑中复杂的PR阵列所产生的功能结果,仍有许多有待发现。此外,临床使用的孕激素以及开发用于大脑靶向结果的选择性PR调节剂的影响是一个关键的研究途径,因为PR的非生殖功能对激素疗法在整个绝经后衰老过程中维持神经健康和功能具有深远影响。