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HtrA3是一种具有胰岛素样生长因子结合结构域的丝氨酸蛋白酶,在小鼠胎盘形成过程中在母胎界面选择性表达。

HtrA3, a serine protease possessing an IGF-binding domain, is selectively expressed at the maternal-fetal interface during placentation in the mouse.

作者信息

Nie G, Li Y, He H, Findlay J K, Salamonsen L A

机构信息

Prince Henry's Institute of Medical Research, PO Box 5152, 246 Clayton Road, Clayton, Victoria 3168, Australia.

出版信息

Placenta. 2006 Apr-May;27(4-5):491-501. doi: 10.1016/j.placenta.2005.03.009. Epub 2005 Jun 13.

Abstract

Hemochorial placentation involves highly regulated interactions between fetal- and maternal-derived cells. HtrA3, a novel serine protease containing an insulin-like growth factor (IGF) binding domain, was previously shown to increase during early pregnancy in the mouse uterus, being dramatically upregulated post-implantation. The present study examined the regulation of HtrA3 gene in the mouse uterus from post-implantation to late gestation. Both mRNA and protein of HtrA3 were localized specifically in the maternal decidua. In contrast, HtrA3 expression was below detection in trophoblasts, including the giant cells that are in direct contact with the decidua. This pattern persisted from the early stages of placentation to near term. The level of decidual HtrA3 mRNA and its protein gradually decreased as the placenta matured. In the decidua, only the maternal decidual cells, but not blood vessels or uterine NK cells that are present in large numbers, were positive for HtrA3. The specific localization of a protease possessing an IGF-binding domain at the maternal-fetal interface suggests that HtrA3 plays a critical role in mediating maternal decidual remodelling and maintenance, likely in association with the IGF system, in placental development and function.

摘要

血绒毛膜胎盘形成涉及胎儿和母体来源细胞之间高度调控的相互作用。HtrA3是一种含有胰岛素样生长因子(IGF)结合域的新型丝氨酸蛋白酶,先前已证明其在小鼠子宫妊娠早期增加,在着床后显著上调。本研究检测了从着床后到妊娠晚期小鼠子宫中HtrA3基因的调控情况。HtrA3的mRNA和蛋白均特异性定位于母体蜕膜。相比之下,HtrA3在滋养层细胞中表达低于检测水平,包括与蜕膜直接接触的巨细胞。这种模式从胎盘形成早期持续到接近足月。随着胎盘成熟,蜕膜HtrA3 mRNA及其蛋白水平逐渐下降。在蜕膜中,只有母体蜕膜细胞对HtrA3呈阳性,而大量存在的血管或子宫NK细胞则呈阴性。在母胎界面具有IGF结合域的蛋白酶的特异性定位表明,HtrA3在介导母体蜕膜重塑和维持中起关键作用,可能与IGF系统相关,参与胎盘发育和功能。

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