Histamine promotes mouse decidualization through stimulating epithelial amphiregulin release

Cheng-Kan Liu, Yu-Ying He, Si-Ting Chen, Wen-Wen Shi, Ying Wang, Hui-Na Luo, Zeng-Ming Yang
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Abstract

Accumulating evidence shows that inflammation is essential for embryo implantation and decidualization. Histamine, a proinflammatory factor that is present in almost all mammalian tissues, is synthesized through decarboxylating histidine by histidine decarboxylase (HDC). Although histamine is known to be essential for decidualization, the underlying mechanism remains undefined. In the present study, histamine had no obvious direct effects on in vitro decidualization in mice. However, the obvious differences in HDC protein levels between day 4 of pregnancy and day 4 of pseudopregnancy, as well as between delayed and activated implantation, suggested that the blastocyst may be involved in regulating HDC expression. Furthermore, blastocyst-derived tumor necrosis factor α (TNFα) significantly increased HDC levels in the luminal epithelium. Histamine increased the levels of amphiregulin (AREG) and disintegrin and metalloproteinase domain-containing protein 17 (ADAM17) proteins, which was abrogated by treatment with famotidine, a specific histamine type 2 receptor (H2R) inhibitor, or by TPAI-1 (a specific inhibitor of ADAM17). Intraluminal injection of urocanic acid (HDC inhibitor) on day 4 of pregnancy significantly reduced the number of implantation sites on day 5 of pregnancy. TNFα-stimulated increases in HDC, AREG and ADAM17 protein levels was abrogated by urocanic acid, a specific inhibitor of HDC. Additionally, AREG treatment significantly promoted in vitro decidualization. Collectively, our data suggests that blastocyst-derived TNFα induces luminal epithelial histamine secretion, and histamine increases mouse decidualization through ADAM17-mediated AREG release.

Abstract Image

组胺通过刺激上皮细胞两性胰岛素的释放来促进小鼠蜕皮。
越来越多的证据表明,炎症对胚胎植入和蜕膜至关重要。组胺是一种几乎存在于所有哺乳动物组织中的促炎因子,通过组氨酸脱羧酶(HDC)将组氨酸脱羧而合成。虽然组胺对蜕膜化至关重要,但其潜在机制仍未确定。在本研究中,组胺对小鼠体外蜕膜化没有明显的直接影响。然而,妊娠第 4 天与假孕第 4 天之间以及延迟着床与激活着床之间 HDC 蛋白水平的明显差异表明,囊胚可能参与调节 HDC 的表达。此外,囊胚衍生的肿瘤坏死因子α(TNFα)会显著增加管腔上皮中的 HDC 水平。组胺会增加安非拉酮(AREG)和含崩解素与金属蛋白酶结构域蛋白17(ADAM17)蛋白的水平,而使用法莫替丁(一种特异性组胺2型受体(H2R)抑制剂)或TPAI-1(一种特异性ADAM17抑制剂)治疗可抑制这种增加。妊娠第 4 天腔内注射尿囊酸(HDC 抑制剂)可显著减少妊娠第 5 天植入点的数量。HDC的特异性抑制剂尿囊酸可抑制TNFα刺激的HDC、AREG和ADAM17蛋白水平的增加。此外,AREG处理可显著促进体外蜕膜化。总之,我们的数据表明囊胚衍生的 TNFα 可诱导管腔上皮组胺分泌,组胺通过 ADAM17 介导的 AREG 释放增加小鼠的蜕膜化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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