4.2 Article Proceedings Paper

Progestin functions in vertebrate gametes mediated by membrane progestin receptors (mPRs): Identification of mPRα on human sperm and its association with sperm motility

Journal

STEROIDS
Volume 74, Issue 7, Pages 614-621

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.steroids.2008.10.020

Keywords

Membrane progestin receptor; Gamete physiology; Oocyte maturation; Human sperm; Sperm motility

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Most of the studies on the putative membrane progestin receptor (mPR) alpha and beta subtypes that have been published in the 5 years since their discovery have supported the original hypothesis that they function as specific membrane receptors through which progestins induce rapid, nongenomic responses in target cells. Recent evidence that mPR alpha and mPR beta have important roles in the regulation of oocyte meiotic maturation and sperm motility in both fish and mammals is reviewed. Although rapid, cell surface-initiated progestin actions on sperm to induce hyperactive motility have been demonstrated in several mammalian models, the identity of the membrane progestin receptor mediating this effect remains unclear. We demonstrate here that mPR alpha mRNA is expressed in human sperm by RT-PCR and that the mPR alpha protein is localized to the sperm membranes by Western blot analysis. Immunocytochemical staining of whole non-permeabilized human sperm confirmed the mPR alpha protein is expressed in the plasma membrane, and showed it is localized to the sperm midpiece, indicating a likely role of mPR alpha in progestin regulation of sperm motility. Moreover, the abundance of the mPR alpha protein on sperm plasma membranes from human donors that displayed low motility was significantly reduced compared to that on normal motile sperm. Finally, progestin treatment of sperm membranes caused activation of G-proteins. These results suggest that, similar to its proposed function in fishes, mPR alpha is an intermediary in progestin stimulation of sperm motility in humans by a mechanism involving G-protein activation. (C) 2008 Elsevier Inc. All rights reserved.

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