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膜孕激素受体α(mPRα)和孕激素膜受体组分1(PGMRC1)的特性及其在介导孕激素快速作用中的作用。

Characteristics of membrane progestin receptor alpha (mPRalpha) and progesterone membrane receptor component 1 (PGMRC1) and their roles in mediating rapid progestin actions.

作者信息

Thomas Peter

机构信息

University of Texas at Austin, Marine Science, 750 Channel View Drive, Port Aransas, TX 78373, USA.

出版信息

Front Neuroendocrinol. 2008 May;29(2):292-312. doi: 10.1016/j.yfrne.2008.01.001. Epub 2008 Feb 1.

Abstract

Rapid, progestin actions initiated at the cell surface that are often nongenomic have been described in a variety of reproductive tissues, but until recently the identities of the membrane receptors mediating these nonclassical progestins actions remained unclear. Evidence has been obtained in the last 4-5 years for the involvement of two types of novel membrane proteins unrelated to nuclear steroid receptors, progesterone membrane receptors (mPRs) and progesterone receptor membrane component 1 (PGMRC1), in progestin signaling in several vertebrate reproductive tissues and in the brain. The mPRs, (M(W) approximately 40 kDa) initially discovered in fish ovaries, comprise at least three subtypes, alpha, beta and gamma and belong to the seven-transmembrane progesterone adiponectin Q receptor (PAQR) family. Both recombinant and wildtype mPRs display high affinity (K(d) approximately 5 nM), limited capacity, displaceable and specific progesterone binding. The mPRs are directly coupled to G proteins and typically activate pertussis-sensitive inhibitory G proteins (G(i)), to down-regulate adenylyl cyclase activity. Recent studies suggest the alpha subtype (mPRalpha) has important physiological functions in variety of reproductive tissues. The mPRalpha is an intermediary in progestin induction of oocyte maturation and stimulation of sperm hypermotility in fish. In mammals, the mPRalphas have been implicated in progesterone regulation of uterine function in humans and GnRH secretion in rodents. The single-transmembrane protein PGMRC1 (M(W) 26-28 kDa) was first purified from porcine livers and its cDNA was subsequently cloned from porcine smooth muscle cells and a variety of other tissues by different investigators. PGMRC1 and the closely-related PGMRC2 belong to the membrane-associated progesterone receptor (MAPR) family. The PGMRC1 protein displays moderately high binding affinity for progesterone which is 2- to 10-fold greater than that for testosterone and glucocorticoids, and also can bind to other molecules such as heme, cholesterol metabolites and proteins. The signal transduction pathways induced by binding of progesterone to PGMRC1 have not been described to date, although motifs for tyrosine kinase, kinase binding, SH2 and SH3 have been predicted from the amino acid sequence. Evidence has been obtained that PGMRC1 mediates the antiapoptotic affects of progesterone in rat granulosa cells. The PGMRC1 protein may also be an intermediary in the progesterone induction of the acrosome reaction in mammalian sperm. Despite these recent advances, many aspects of progestin signaling through these two families of novel membrane proteins remain unresolved. Biochemical characterization of the receptors has been hampered by rapid degradation of the partially purified proteins. A major technical challenge has been to express sufficient amounts of the recombinant receptors on the plasma membranes in eukaryotic systems to permit investigations of their progestin binding and signal transduction characteristics. Additional basic information on the molecular and cellular mechanisms by which mPRs and PGMRC1 interact with progestins, signal transductions pathways and other proteins will be required to establish a comprehensive model of nontraditional progestin actions mediated through these novel proteins.

摘要

在多种生殖组织中,已经描述了在细胞表面启动的快速孕激素作用,这些作用通常是非基因组的,但直到最近,介导这些非经典孕激素作用的膜受体的身份仍不清楚。在过去的4到5年中,已经获得证据表明,两种与核类固醇受体无关的新型膜蛋白,即孕激素膜受体(mPRs)和孕激素受体膜成分1(PGMRC1),参与了几种脊椎动物生殖组织和大脑中的孕激素信号传导。mPRs(分子量约40 kDa)最初在鱼卵巢中发现,至少包括三个亚型,α、β和γ,属于七跨膜孕激素脂联素Q受体(PAQR)家族。重组型和野生型mPRs均显示出高亲和力(解离常数约5 nM)、有限容量、可置换且特异性的孕激素结合。mPRs直接与G蛋白偶联,通常激活对百日咳敏感的抑制性G蛋白(G(i)),以下调腺苷酸环化酶活性。最近的研究表明,α亚型(mPRα)在多种生殖组织中具有重要的生理功能。mPRα是鱼类中孕激素诱导卵母细胞成熟和刺激精子超激活运动的中间介质。在哺乳动物中,mPRαs与人类子宫功能的孕激素调节以及啮齿动物促性腺激素释放激素(GnRH)的分泌有关。单跨膜蛋白PGMRC1(分子量26 - 28 kDa)最初从猪肝中纯化出来,随后不同的研究人员从猪平滑肌细胞和多种其他组织中克隆了其cDNA。PGMRC1和密切相关的PGMRC2属于膜相关孕激素受体(MAPR)家族。PGMRC1蛋白对孕激素表现出中等程度的高结合亲和力,比对睾酮和糖皮质激素的亲和力高2至10倍,并且还可以与其他分子如血红素、胆固醇代谢产物和蛋白质结合。尽管从氨基酸序列预测了酪氨酸激酶、激酶结合、SH2和SH3基序,但迄今为止,尚未描述孕激素与PGMRC1结合所诱导的信号转导途径。已经获得证据表明,PGMRC1介导了孕激素在大鼠颗粒细胞中的抗凋亡作用。PGMRC1蛋白也可能是哺乳动物精子中孕激素诱导顶体反应的中间介质。尽管有这些最新进展,但通过这两类新型膜蛋白进行的孕激素信号传导的许多方面仍未解决。受体的生化特性研究因部分纯化蛋白的快速降解而受阻。一个主要的技术挑战是在真核系统的质膜上表达足够量的重组受体,以允许研究它们的孕激素结合和信号转导特性。需要关于mPRs和PGMRC1与孕激素相互作用的分子和细胞机制、信号转导途径以及其他蛋白质的更多基础信息,以建立通过这些新型蛋白介导的非传统孕激素作用的综合模型。

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