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人 MUC1 在人 MUC1 转基因小鼠模型早孕中的表达。

Expression of human MUC1 during early pregnancy in the human MUC1 transgenic mouse model.

机构信息

Department of Biological Sciences, University of Delaware, Newark, Delaware, USA.

出版信息

Biol Reprod. 2009 Dec;81(6):1182-8. doi: 10.1095/biolreprod.109.079418. Epub 2009 Aug 14.

Abstract

Embryo implantation involves direct interaction of the blastocyst with the luminal epithelium of the receptive uterus. MUC1, a transmembrane mucin expressed at the apical surface of uterine epithelia, acts as a barrier to microbial infection and enzymatic attack. Loss of MUC1 is believed to be a prerequisite for a functionally receptive uterus across many species. Human and murine MUC1 regulation by steroid hormones displays important differences. Estrogen (E2) stimulates MUC1 expression in mice, and progesterone (P4) antagonizes E2 action in this regard. MUC1 expression is severely reduced during the receptive uterine state in mice. In contrast, human MUC1 expression is maximal at the receptive or midluteal phase, when P4 levels are high. No information is available regarding regulation of human MUC1 in vivo at the site of embryo attachment. Our aim was to better understand regulation of human MUC1 during early pregnancy in vivo. For this purpose, we used a transgenic mouse carrying full-length human MUC1 gene (Tg(MUC1)79.24Gend) as well as endogenous MUC1 as a model system. Human MUC1 was detected by real-time RT-PCR, Western blotting, and immunohistochemistry during early pregnancy. Our data indicate that human MUC1 persists at reduced (20% relative to Day 1 postcoitum) levels in receptive-phase uteri, including the site of embryo attachment. In contrast, mouse MUC1 was much more severely (>98% relative to Day 1 postcoitum) reduced in the same context. These observations are consistent with distinct regulation between the human and mouse genes. Because these genes are expressed in the same transcriptional context (i.e., mouse uterine epithelia), structural differences between human and murine genes must account for these differences in MUC1 regulation.

摘要

胚胎着床涉及囊胚与接受性子宫腔上皮的直接相互作用。MUC1 是一种在子宫上皮顶表面表达的跨膜粘蛋白,作为微生物感染和酶攻击的屏障。据信,MUC1 的丧失是许多物种功能性接受性子宫的先决条件。类固醇激素对人和鼠 MUC1 的调节存在重要差异。雌激素(E2)刺激小鼠的 MUC1 表达,而孕激素(P4)在这方面拮抗 E2 的作用。在小鼠的接受性子宫状态下,MUC1 的表达严重减少。相比之下,人类 MUC1 的表达在接受期或黄体中期达到最大值,此时 P4 水平较高。关于胚胎附着部位人 MUC1 的体内调节尚无信息。我们的目的是更好地了解人 MUC1 在体内早期妊娠期间的调节。为此,我们使用携带全长人 MUC1 基因(Tg(MUC1)79.24Gend)的转基因小鼠以及内源性 MUC1 作为模型系统。在早期妊娠期间通过实时 RT-PCR、Western 印迹和免疫组织化学检测人 MUC1。我们的数据表明,人 MUC1 在接受期子宫(包括胚胎附着部位)中以降低的水平(相对于交配后第 1 天的 20%)持续存在。相比之下,在相同的情况下,鼠 MUC1 减少了更多(相对于交配后第 1 天的 98%)。这些观察结果与人和鼠基因之间的不同调节一致。由于这些基因在相同的转录背景下表达(即,小鼠子宫上皮),人基因和鼠基因之间的结构差异必须解释 MUC1 调节的这些差异。

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