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Heterologous expression of human mPRα mPRβ and mPRγ in yeast confirms their ability to function as membrane progesterone receptors

机译:人mPRαmPRβ和mPRγ在酵母中的异源表达证实了它们具有作为膜孕激素受体的功能

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摘要

The nuclear progesterone receptor (nPR) mediates many of the physiological effects of progesterone by regulating the expression of genes, however, progesterone also exerts non-transcriptional (non-genomic) effects that have been proposed to rely on a receptor that is distinct from nPR. Several members of the Progestin and AdipoQ Receptor (PAQR) family were recently identified as potential mediators of these non-genomic effects. Membranes from cells expressing these proteins, called mPRα, mPRβ and mPRγ, were shown to specifically bind progesterone and have G-protein coupled receptor (GPCR) characteristics, although other studies dispute these findings. To clarify the role of these mPRs in non-genomic progesterone signaling, we established an assay for PAQR functional evaluation using heterologous expression in Saccharomyces cerevisiae. Using this assay, we demonstrate unequivocally that mPRα, mPRβ and mPRγ can sense and respond to progesterone with EC50 values that are physiologically relevant. Agonist profiles also show that mPRα, mPRβ and mPRγ are activated by ligands, such as 17α-hydroxyprogesterone, that are known to activate non-genomic pathways but not nPR. These results strongly suggest that these receptors may indeed function as the long-sought-after membrane progesterone receptors. Additionally, we show that two uncharacterized PAQRs, PAQR6 and PAQR9, are also capable of responding to progesterone. These mPR-like PAQRs have been renamed mPRδ (PAQR6) and mPRε (PAQR9). Additional characterization of mPRγ and mPRα indicate that their progesterone-dependent signaling in yeast does not require heterotrimeric G-proteins, thus calling into question the characterization of the mPRs as a novel class of G-protein coupled receptor.
机译:核孕酮受体(nPR)通过调节基因的表达来介导孕酮的许多生理作用,但是,孕酮还发挥非转录(非基因组)作用,该作用被认为依赖于不同于nPR的受体。孕激素和AdipoQ受体(PAQR)家族的几个成员最近被确定为这些非基因组效应的潜在介质。表达其他蛋白质的细胞膜(称为mPRα,mPRβ和mPRγ)被证明与孕激素特异性结合,并具有G蛋白偶联受体(GPCR)特性,尽管其他研究对此提出了质疑。为了阐明这些mPR在非基因组孕酮信号传导中的作用,我们建立了一种在酿酒酵母中使用异源表达进行PAQR功能评估的方法。使用该测定法,我们明确证明了mPRα,mPRβ和mPRγ可以以生理相关的EC50值来感知并响应孕酮。激动剂谱还显示,mPRα,mPRβ和mPRγ被已知为激活非基因组途径但不激活nPR的配体(例如17α-羟基孕酮)激活。这些结果有力地表明,这些受体确实可以作为人们期待已久的膜孕酮受体。此外,我们显示两个未表征的PAQRs,PAQR6和PAQR9,也能够对孕激素作出反应。这些类似于mPR的PAQR已重命名为mPRδ(PAQR6)和mPRε(PAQR9)。 mPRγ和mPRα的其他特征表明它们在酵母中依赖孕激素的信号传导不需要异三聚体G蛋白,因此,人们质疑mPRs作为新型G蛋白偶联受体的特征。

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