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首页> 外文期刊>Cell & Bioscience >Secretory phospholipase A2-X ( Pla2g10 ) is a novel progesterone receptor target gene exclusively induced in uterine luminal epithelium for uterine receptivity in mice
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Secretory phospholipase A2-X ( Pla2g10 ) is a novel progesterone receptor target gene exclusively induced in uterine luminal epithelium for uterine receptivity in mice

机译:分泌磷脂酶A2-X(PLA2G10)是专门在小鼠中有子宫腔上皮中诱导的新型孕酮受体靶基因。

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摘要

Aberration of estrogen (E2) and/or progesterone (P4) signaling pathways affects expression of their target genes, which may lead to failure of embryo implantation and following pregnancy. Although many target genes of progesterone receptors (PRs) have been identified in uterine stroma, only a few PR targets have been reported in the epithelium. Secretory phospholipase A2-(PLA2)-X, a member of the PLA2 family that releases arachidonic acids for the synthesis of prostaglandins that are important for embryo implantation, is dysregulated in the endometrium of patients suffering from repeated implantation failure. However, it is not clear whether sPLA2-X is directly regulated by ovarian steroid hormones for embryo implantation in the uterus. P4 induced the Pla2g10 encoding of secretory PLA2-X in the apical region of uterine LE of ovariectomized mice via PR in both time- and dose-dependent manners, whereas E2 significantly inhibited it. This finding is consistent with the higher expression of Pla2g10 at the diestrus stage, when P4 is elevated during the estrous cycle, and at P4-treated delayed implantation. The level of Pla2g10 on day 4 of pregnancy (day 4) was dramatically decreased on day 5, when PRs are absent in the LE. Luciferase assays of mutagenesis in uterine epithelial cells demonstrated that four putative PR response elements in a Pla2g10 promoter region are transcriptionally active for Pla2g10. Intrauterine delivery of small interfering RNA for Pla2g10 on day 3 significantly reduced the number of implantation sites, reinforcing the critical function(s) of Pla2g10 for uterine receptivity in mice. Pla2g10 is a novel PR target gene whose expression is exclusively localized in the apical region of the uterine LE for uterine receptivity for embryo implantation in mice.
机译:雌激素(E2)和/或孕酮(P4)信号传导途径的像差会影响其靶基因的表达,这可能导致胚胎植入和怀孕后的失效。虽然在子宫基质中鉴定了孕酮受体(PRS)的许多靶基因,但上皮内仅报道了几种PR靶标。分泌磷脂酶A2-(PLA2)-X,PLA2系列的成员,其释放用于合成前列腺素对胚胎植入的前列腺素的合成,在患有重复植入失败的患者的子宫内膜中失去了测定。然而,目前尚不清楚SPLA2-X是否由卵巢类固醇激素直接调节,用于在子宫内胚胎植入。 P4通过PR在两种时间和剂量依赖的举射中诱导PLA2G10在卵巢切除小鼠的子宫杆的顶端区域中的分泌物PLA2-X编码,而E2显着抑制它。当在溶解循环期间P4升高时,该发现与Diestrus阶段的PLA2G10的表达较高,并且在P4处理的延迟注入时,P4升高。在怀孕第4天(第4天)的PLA2G10水平在第5天发生显着降低,当时PRS在LE中不存在。子宫上皮细胞中诱变的荧光素酶测定证明了PLA2G10启动子区中的四个推定的PR响应元件用于PLA2G10的转录活性。在第3天的PLA2G10中小干扰RNA的宫内递送显着降低了植入位点的数量,增强了小鼠中子宫接收性PLA2G10的临界功能。 PLA2G10是一种新的PR靶基因,其表达专用于子宫lef的子宫lef的子宫接受,用于小鼠中的胚胎植入物。

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