2002
DOI: 10.1530/rep.0.1240167
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Anti-proliferative effects of progesterone antagonists in the primate endometrium: a potential role for the androgen receptor

Abstract: In women and non-human primates, treatment with anti-progestins suppresses oestrogen-dependent mitotic activity in the endometrial glands. This anti-proliferative effect is paradoxical, because anti-progestins do not bind to the oestrogen receptor. Although this phenomenon has been termed a 'non-competitive anti-oestrogenic effect', it does not occur in all species or in other regions of the primate reproductive tract, so is best referred to as an 'endometrial anti-proliferative effect'. The abundance of andro… Show more

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Cited by 55 publications
(12 citation statements)
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“…Pathway analysis is widely used to analyze gene expression data and serves as an effective tool for delineating the underlying biological processes involved in mRNA aberrations [6871]. Biological pathways altered in the current study included: cellular growth and proliferation, lipid metabolism, tissue remodeling, ECM mineralization, inflammation, angiogenesis, and metabolic exchange.…”
Section: Discussionmentioning
confidence: 99%
“…Pathway analysis is widely used to analyze gene expression data and serves as an effective tool for delineating the underlying biological processes involved in mRNA aberrations [6871]. Biological pathways altered in the current study included: cellular growth and proliferation, lipid metabolism, tissue remodeling, ECM mineralization, inflammation, angiogenesis, and metabolic exchange.…”
Section: Discussionmentioning
confidence: 99%
“…80,81 Since androgens suppress estrogen-induced endometrial proliferation, the increase in the AR could be a possible mechanism to explain the antiproliferative effects. 82 In the presence of mifepristone, receptors adopt an inactive conformation and preferentially interact with corepressors such as nuclear receptor corepressor and silencing mediator of retinoic acid and thyroid hormone, resulting in loss of transcriptional activity. 83 The mixed agonist/antagonist, asoprisnil (that are a selective PR modulator for gynecological therapy), partially recruits coactivators and strongly recruits corepressors, 84 which explains its mixed agonist and antagonist action.…”
Section: Genomic Pathways Of Mifepristonementioning
confidence: 99%
“…However, the increase in estrogen and PRs is also associated with an increase in the number of androgen receptor. [80][81][82] Since androgens suppress estrogeninduced endometrial proliferation, the increase in the AR could be a possible mechanism to explain the antiproliferative effects. Further evidence of the role played by androgens in this antiproliferative effect is the observation that the specific nuclear antagonist of the AR, flutamide, blocks the antiproliferative effects in the endometrium.…”
Section: Genomic Pathways Of Mifepristonementioning
confidence: 99%
“…Long-term administration of low doses of antiprogestin (RU486) allowed normal ovarian cycles, but suppressed endometrial growth and decreased glandular cell proliferation in women, demonstrating that the endometrium was more sensitive to the effects of anti-progestin than were other tissues (Cameron et al 1996). In primates, the anti-progestin (ZK 137136) inhibited endometrial mitotic activity, wet mass and thickness, and suppressed endometrial growth and glandular proliferation (Brenner et al 2002), whereas in rodents, anti-progestins did not cause any anti-proliferative effects in the oviductal or vaginal epithelium (Chwalisz et al 1998). The antagonism to the action of progesterone in regression of the mammary tissue has been reported in cats developing fibroadenomatous hyperplasia, when aglepristone is given at 10 mg ⁄ kg on four to five consecutive days (Wehrend et al 2001).…”
Section: Discussionmentioning
confidence: 99%