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细胞与上皮顶端的黏附:细胞极性的一种功能。

Cell adhesion to the apical pole of epithelium: a function of cell polarity.

作者信息

Thie M, Harrach-Ruprecht B, Sauer H, Fuchs P, Albers A, Denker H W

机构信息

Institute of Anatomy, University of Essen, Medical School, Germany.

出版信息

Eur J Cell Biol. 1995 Feb;66(2):180-91.

PMID:7774604
Abstract

Human uterine epithelium displays a distinct polarized organization with apical, lateral, and basal plasma membrane domains. Although non-adhesive throughout most of the menstrual cycle, epithelial cells allow attachment of trophoblast cells to their apical pole during embryo implantation. A recent hypothesis postulates that epithelial cells turn off genes for apical-basal polarity and turn on genes for a more mesenchyme-like phenotype allowing cell-cell interaction with trophoblast. Using an in vitro assay human uterine cell lines (RL95-2, HEC-1-A, AN3-CA) were selected on the basis of adhesiveness for trophoblast-type cells (JAR). Subsequently, uterine cells were examined for epithelium-specific ultrastructure using transmission electron microscopy, and for the expression of E-cadherin, alpha 6-, beta 1-, beta 4-integrin subunits and cytokeratin using immunocytochemistry, confocal laser scanning microscopy, and surface replication technique. HEC-1-A monolayers are non-adhesive for JAR cells and appear highly polarized expressing E-cadherin, alpha 6-, beta 1-, beta 4-integrin subunits, and cytokeratin. Both, integrins and E-cadherin, are present at the lateral membrane. RL95-2 monolayers which are adhesive for JAR cells appear non-polarized. Like HEC-1-A cells, RL95-2 cells express E-cadherin, alpha 6-, beta 1-, and beta 4-integrin subunits, and cytokeratin. In contrast to HEC-1-A cells, integrins and E-cadherin are distributed at the entire cell surface. AN3-CA monolayers are non-adhesive for JAR cells and appear non-polarized. Cells lack epithelial-specific markers such as keratin and E-cadherin. They show only low expression of alpha 6-, beta 1-integrin subunits and lack beta 4-integrin subunit. Conversely, they express vimentin. Thus, modulation of the epithelial phenotype of uterine cells, i.e. loss of apical-basal polarity, might prepare the apical cell pole for cell-cell interaction with trophoblast. However, loss of cell polarity would not lead to enhancement of adhesiveness for trophoblast if accompanied by a loss of epithelium-specific adhesion molecules.

摘要

人子宫内膜上皮呈现出独特的极化组织,具有顶端、侧面和基底质膜结构域。尽管在月经周期的大部分时间里不具有黏附性,但在胚胎植入期间,上皮细胞允许滋养层细胞附着于其顶端极。最近的一个假说是,上皮细胞关闭顶端 - 基底极性相关基因,并开启更具间充质样表型的基因,从而允许与滋养层细胞进行细胞间相互作用。使用体外试验,根据对滋养层型细胞(JAR)的黏附性选择人子宫细胞系(RL95 - 2、HEC - 1 - A、AN3 - CA)。随后,使用透射电子显微镜检查子宫细胞的上皮特异性超微结构,并使用免疫细胞化学、共聚焦激光扫描显微镜和表面复制技术检查E - 钙黏蛋白、α6 -、β1 -、β4 -整合素亚基和细胞角蛋白的表达。HEC - 1 - A单层细胞对JAR细胞不具有黏附性,并且呈现高度极化,表达E - 钙黏蛋白、α6 -、β1 -、β4 -整合素亚基和细胞角蛋白。整合素和E - 钙黏蛋白均存在于侧面膜上。对JAR细胞具有黏附性的RL95 - 2单层细胞似乎没有极化。与HEC - 1 - A细胞一样,RL95 - 2细胞表达E - 钙黏蛋白、α6 -、β1 -和β4 -整合素亚基以及细胞角蛋白。与HEC - 1 - A细胞不同,整合素和E - 钙黏蛋白分布在整个细胞表面。AN3 - CA单层细胞对JAR细胞不具有黏附性,并且似乎没有极化。细胞缺乏上皮特异性标志物,如角蛋白和E - 钙黏蛋白。它们仅显示α6 -、β1 -整合素亚基的低表达,并且缺乏β4 -整合素亚基。相反,它们表达波形蛋白。因此,子宫细胞上皮表型的调节,即顶端 - 基底极性的丧失,可能为与滋养层细胞的细胞间相互作用准备顶端细胞极。然而,如果伴随着上皮特异性黏附分子的丧失,细胞极性的丧失不会导致对滋养层细胞黏附性的增强。

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