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子宫表面的再上皮化源于子宫内膜腺体:来自破坏和修复功能小鼠模型的证据。

Reepithelialization of the uterine surface arises from endometrial glands: evidence from a functional mouse model of breakdown and repair.

机构信息

The Ritchie Centre, MIMR, 27-31 Wright Street, Clayton, Victoria 3168, Australia.

出版信息

Endocrinology. 2010 Jul;151(7):3386-95. doi: 10.1210/en.2009-1334. Epub 2010 May 5.

Abstract

The human endometrium is highly regenerative undergoing monthly cycles of growth and regression. Endometrial repair after menses is a critical component of the cycle; however, little is understood about the mechanisms behind this rapid process. Adult stem/progenitor cells identified in human and mouse endometrium may be responsible for its remarkable regenerative capacity; however, a functional role for stem/progenitor cells in menstruation is yet to be established. This study aimed to identify label retaining cells as candidate epithelial stem or progenitor cells involved in the rapid reepithelization of the uterine surface in our functional mouse model of endometrial breakdown and repair. Adult mice were pulse labeled with bromodeoxyuridine before endometrial breakdown and repair was induced. Throughout endometrial breakdown and repair, very rapid dilution of bromodeoxyuridine label was observed in the luminal epithelium, whereas label within the glandular epithelium remained constant. Importantly, glandular epithelial cells were shown to proliferate selectively in response to endometrial repair, and the majority strongly expressed estrogen receptor-alpha at this time. This is the first study to demonstrate a functionally diverse response during endometrial repair from the anatomically connected luminal and glandular epithelium and highlights the likelihood that the endometrial glands are the residence of epithelial progenitor cells contributing to reepithelialization of the uterine surface after menses.

摘要

人类子宫内膜具有高度再生能力,每月经历生长和退化的循环。月经后子宫内膜的修复是周期的关键组成部分;然而,对于这个快速过程的机制知之甚少。在人类和小鼠子宫内膜中鉴定出的成人干细胞/祖细胞可能负责其显著的再生能力;然而,干细胞/祖细胞在月经中的功能作用尚未确定。本研究旨在鉴定标记保留细胞作为候选上皮干细胞或祖细胞,参与我们功能性小鼠模型中子宫内膜破裂和修复过程中子宫表面的快速再上皮化。在子宫内膜破裂和修复之前,用溴脱氧尿苷对成年小鼠进行脉冲标记。在整个子宫内膜破裂和修复过程中,在腔上皮中观察到溴脱氧尿苷标记的快速稀释,而在腺上皮中标记保持不变。重要的是,已经表明腺上皮细胞选择性地增殖以响应子宫内膜修复,并且此时大多数强烈表达雌激素受体-α。这是第一项研究,从解剖上连接的腔上皮和腺上皮中证明了在子宫内膜修复过程中具有功能多样性的反应,并强调了子宫内膜腺体可能是在月经后有助于子宫表面再上皮化的上皮祖细胞的栖息地。

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