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Endometrial cysteine-rich secretory protein 3 is inhibited by human chorionic gonadotrophin and is increased in the decidua of tubal ectopic pregnancy

机译:子宫内膜富含半胱氨酸的分泌蛋白3被绒毛膜促性腺激素抑制并在输卵管异位妊娠的蜕膜中增加

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摘要

Ectopic pregnancy (EP) remains a considerable cause of morbidity and occasional mortality. Currently, there is no reliable test to differentiate ectopic from intrauterine gestation. We have previously used array technology to demonstrate that differences in gene expression in decidualized endometrium from women with ectopic and intrauterine gestations could be used to identify candidate diagnostic biomarkers for EP. The aim of this study was to further investigate the decidual gene with the highest fold increase in EP, cysteine-rich secretory protein-3 (CRISP-3). Decidualized endometrium from gestation-matched women undergoing surgical termination of pregnancy (n = 8), evacuation of uterus for miscarriage (n = 6) and surgery for EP (n = 11) was subjected to quantitative RT–PCR, morphological assessment, immunohistochemistry and western blot analysis. Sera were analysed for progesterone and human chorionic gonadotrophin (hCG) levels. Immortalized endometrial epithelial cells were cultured with physiological concentrations of hCG. CRISP-3 mRNA and protein expression were greater in endometrium from ectopic when compared with intrauterine pregnancies (P < 0.05). CRISP-3 protein was localized to epithelium and granulocytes of endometrium. CRISP-3 serum concentrations were not different in women with ectopic compared with intrauterine pregnancies. CRISP-3 expression in endometrium was not related to the degree of decidualization or to serum progesterone levels. Endometrial CRISP-3 expression was inversely proportional to serum hCG concentrations (P < 0.001). Stimulation of endometrial epithelial cells with hCG in vitro caused a reduction in CRISP-3 expression (P < 0.01). The measurement of CRISP-3 in endometrium could provide an additional tool in the diagnosis of failing early pregnancy of unknown location. The absence of a local reduction in expression of CRISP-3 in decidualized endometrium of women with EP may be due to reduced exposure to hCG due to the ectopic location of the trophoblast.
机译:异位妊娠(EP)仍然是发病率和偶发性死亡的重要原因。目前,尚无可靠的测试可将异位与宫内妊娠区分开。我们以前曾使用阵列技术来证明异位妊娠和宫内妊娠妇女蜕膜化子宫内膜基因表达的差异可用于鉴定EP的候选诊断性生物标志物。这项研究的目的是进一步研究在EP中富含半胱氨酸的分泌蛋白3(CRISP-3)具有最高倍数增加的蜕膜基因。对经过妊娠终止手术的妊娠匹配妇女的子宫内膜蜕膜(n = 8),流产子宫排空(n = 6)和EP手术(n = 11)进行了定量RT-PCR,形态学评估,免疫组化和免疫印迹分析。分析血清中的孕激素和人绒毛膜促性腺激素(hCG)水平。用生理浓度的hCG培养永生化的子宫内膜上皮细胞。与宫内妊娠相比,异位子宫内膜的CRISP-3 mRNA和蛋白表达更高(P <0.05)。 CRISP-3蛋白定位于子宫内膜的上皮和粒细胞。与宫内妊娠相比,异位妇女的CRISP-3血清浓度没有差异。子宫内膜中CRISP-3的表达与蜕膜化程度或血清孕激素水平无关。子宫内膜CRISP-3表达与血清hCG浓度成反比(P <0.001)。 hCG体外刺激子宫内膜上皮细胞导致CRISP-3表达降低(P <0.01)。子宫内膜CRISP-3的测量可为诊断未知部位失败的早期妊娠失败提供额外的工具。患有EP的女性蜕膜化子宫内膜中CRISP-3的表达没有局部降低可能是由于滋养细胞的异位导致接触hCG的减少。

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