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首页> 外文期刊>Gynecological endocrinology: the official journal of the International Society of Gynecological Endocrinology >Association between prolactin receptor expression and proliferation in the endometrium of obese women with polycystic ovary syndrome
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Association between prolactin receptor expression and proliferation in the endometrium of obese women with polycystic ovary syndrome

机译:多囊卵巢综合征肥胖妇女子宫内膜催乳素受体表达与增殖的关系

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摘要

Polycystic ovary syndrome (PCOS) is associated with increased risk of endometrial cancer. There is growing evidence that prolactin and its receptor (PRLR) are involved in the development of cancer. We assessed endometrial expression of PRLR mRNA, and immunostaining of PRLR and the proliferation marker Ki67 on different cycle days in obese (OB-PCOS) and normal-weight women with PCOS and body mass index-matched controls. The OB-PCOS group underwent a 3 months lifestyle intervention. Prior to intervention, obese women with PCOS and controls had lower endometrial levels of PRLR mRNA in proliferative endometrium than the normal-weight groups (p < .05). After intervention, six OB-PCOS women had confirmed ovulation, while 12 remained anovulatory. Both these subgroups displayed higher immunostaining of PRLR in endometrial stroma, and in the anovulatory subgroup also increased Ki67, on cycle days 21-23 compared with controls (p < .05). In obese controls, the PRLR mRNA expression was decreased in secretory endometrium compared with proliferative endometrium (p = .004). A corresponding change within the cycle was not found in OB-PCOS women. Immunostaining of PRLR in the secretory phase correlated positively with Ki67 (p < .05) in the endometrium. These observations suggest that short-term lifestyle intervention can restore ovulation but not normalize PRLR expression in the endometrium of obese women with PCOS. Trial registration: ISRCTN, ISRCTN18400086,
机译:多囊卵巢综合征(PCOS)与子宫内膜癌的风险增加有关。促使催乳素及其受体(PRLR)的越来越多的证据参与了癌症的发展。我们评估了PRLR mRNA的子宫内膜表达,PRLR和PRL​​R的免疫染色和增殖标志物KI67在肥胖(OB-PCOS)和具有PCOS和体重指数匹配对照的正常重量妇女的不同循环天。 OB-PCOS组经历了3个月的生活方式干预。在干预之前,具有PCOS和对照的肥胖女性在增殖子宫内膜中具有低于正常重量基团的PRLR mRNA的子宫内膜水平(P <.05)。干预后,六个ob-pcos女性确认排卵,而12仍保持稳压。这些亚组在子宫内膜基质中显示出更高的PRLR免疫染色,并且在与对照组(P <0.05)相比的循环天21-23上也增加了Ki67的ki67。在肥胖对照中,与增殖子宫内膜相比,分泌子宫内膜中PRLR mRNA表达降低(P = .004)。在ob-pcos女性中找不到循环内的相应变化。 PRLR在分泌阶段中的免疫染色与子宫内膜中的Ki67(P <.05)正相关。这些观察结果表明,短期的生活方式干预可以恢复排卵,但未使PCOS的肥胖女性的子宫内膜中的PRLR表达正常化。试用注册:ISRCTN,ISRCTN18400086,

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