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 Non-genomic progesterone actions in female reproduction Gellersen B; Fernandes MS; Brosens JJHum Reprod Update  2009[Jan]; 15 (1): 119-38BACKGROUND: The steroid hormone progesterone is indispensable for mammalian  procreation by controlling key female reproductive events that range from  ovulation to implantation, maintenance of pregnancy and breast development. In  addition to activating the progesterone receptors (PRs)-B and -A, members of the  superfamily of ligand-dependent transcription factors, progesterone also elicits  a variety of rapid signalling events independently of transcriptional or genomic  regulation. This review covers our current knowledge on the mechanisms and  relevance of non-genomic progesterone signalling in female reproduction. METHODS:  PubMed was searched up to August 2008 for papers on progesterone actions in  ovary/breast/endometrium/myometrium/brain, focusing primarily on non-genomic  signalling mechanisms. RESULTS: Convergence and intertwining of rapid non-genomic  events and the slower transcriptional actions critically determine the functional  response to progesterone in the female reproductive system in a cell-type- and  environment-specific manner. Several putative progesterone-binding moieties have  been implicated in rapid signalling events, including the 'classical' PR and its  variants, progesterone receptor membrane component 1, and the novel family of  membrane progestin receptors. Progesterone and its metabolites have also been  implicated in the allosteric regulation of several unrelated receptors, such as  gamma-aminobutyric acid type A, oxytocin and sigma(1) receptors. CONCLUSIONS:  Identification of the mechanisms and receptors that relay rapid progesterone  signalling is an area of research fraught with difficulties and controversy. More  in-depth characterization of the putative receptors is required before the  non-genomic progesterone pathway in normal and pathological reproductive function  can be targeted for pharmacological intervention.|Brain/metabolism[MESH]|Breast/metabolism[MESH]|Endometrium/metabolism[MESH]|Female[MESH]|Genome, Human[MESH]|Humans[MESH]|Myometrium/metabolism[MESH]|Ovary/metabolism[MESH]|Progesterone/metabolism/*physiology[MESH]|Receptors, Progesterone/physiology[MESH]|Reproduction/*physiology[MESH]|Signal Transduction[MESH]
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