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小鼠胚胎着床时整合素表达的发育调控。

Developmental regulation of integrin expression at the time of implantation in the mouse embryo.

作者信息

Sutherland A E, Calarco P G, Damsky C H

机构信息

Department of Stomatology, University of California San Francisco 94143.

出版信息

Development. 1993 Dec;119(4):1175-86. doi: 10.1242/dev.119.4.1175.

Abstract

The trophectoderm layer of the mouse blastocyst differentiates at the late blastocyst stage to form the invasive trophoblast that mediates implantation of the embryo into the uterine wall. The first sign that trophoblast cells have developed an invasion-specific cell behavior appears about 10-15 hours after the embryo hatches from the zona pellucida, when the quiescent, non-adherent trophectoderm cells initiate protrusive activity and become adhesive to extracellular matrix. Our previous findings that trophoblast outgrowth on extracellular-matrix-coated substrata involves the integrin family of adhesion receptors (Sutherland, A. E., Calarco, P. G. and Damsky, C. H., 1988, J. Cell Biol. 106, 1331-1348), suggested that the onset of trophoblast adhesive and migratory behavior at the time of implantation may be due to changes in expression or distribution of integrin receptors. We have thus examined the mRNA and protein expression of individual integrin subunits during pre- and periimplantation development (E0-E7.5). A basic repertoire of integrins, including receptors for fibronectin (alpha 5 beta 1), laminin (alpha 6B beta 1) and vitronectin (alpha v beta 3), was expressed continuously throughout this period, whereas the expression of five other integrin subunits was developmentally regulated. The mRNA for three of these (alpha 2, alpha 6A and alpha 7) was first detected in the late blastocyst, coincident with endoderm differentiation and development of attachment competence. The mRNA for another (alpha 1) was not detected until after trophoblast outgrowth had begun, suggesting that its expression may be induced by contact with matrix. At E7.5, three of the temporally regulated integrins (alpha 1, apha 6A, alpha 7), all of which can form receptors for laminin, were detected only in the ectoplacental cone (differentiating trophoblast), and may thus play specific roles in trophoblast adhesion and/or differentiation. Because laminin expression is upregulated in decidualized uterine stroma in response to the implanting embryo, we examined trophoblast-laminin interactions, using laminin fragments and integrin antibodies to determine which integrin receptors were involved. Trophoblast cells attached and spread on both the E8 and P1' fragments of laminin; however, the P1' binding site was cryptic in intact laminin. Interaction with P1' was RGD- and alpha v beta 3-dependent, whereas outgrowth on E8 was RGD-independent and not inhibited by antibodies to the laminin receptor alpha 6 beta 1, suggesting that alpha 7 beta 1 is the major trophoblast integrin E8 receptor.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

小鼠囊胚的滋养外胚层在囊胚晚期分化,形成侵袭性滋养层,介导胚胎植入子宫壁。滋养层细胞出现侵袭特异性细胞行为的首个迹象,大约在胚胎从透明带孵化后10 - 15小时出现,此时静止、不黏附的滋养外胚层细胞开始产生突出活动,并变得对细胞外基质具有黏附性。我们之前的研究发现,在细胞外基质包被的基质上滋养层细胞的生长涉及黏附受体的整合素家族(萨瑟兰,A.E.,卡拉尔科,P.G.和丹姆斯基,C.H.,1988年,《细胞生物学杂志》106卷,1331 - 1348页),这表明植入时滋养层黏附及迁移行为的起始可能归因于整合素受体表达或分布的变化。因此,我们检测了植入前和植入周围发育阶段(E0 - E7.5)各个整合素亚基的mRNA和蛋白质表达。在整个这一时期持续表达整合素的一个基本组成部分,包括纤连蛋白受体(α5β1)、层粘连蛋白受体(α6Bβ1)和玻连蛋白受体(αvβ3),而其他五个整合素亚基的表达则受到发育调控。其中三个亚基(α2、α6A和α7)的mRNA首次在囊胚晚期被检测到,与内胚层分化及附着能力的发育同时出现。另一个亚基(α1)的mRNA直到滋养层细胞开始生长后才被检测到,这表明其表达可能由与基质的接触诱导。在E7.5时,三个受时间调控的整合素(α1、α6A、α7),它们都能形成层粘连蛋白受体,仅在外胎盘锥(分化的滋养层)中被检测到,因此可能在滋养层黏附和/或分化中发挥特定作用。由于层粘连蛋白的表达在蜕膜化的子宫基质中因植入胚胎而上调,我们利用层粘连蛋白片段和整合素抗体检测了滋养层 - 层粘连蛋白的相互作用,以确定涉及哪些整合素受体。滋养层细胞在层粘连蛋白的E8和P1'片段上附着并铺展;然而,P1'结合位点在完整的层粘连蛋白中是隐蔽的。与P1'的相互作用依赖于RGD和αvβ3,而在E8上的生长不依赖于RGD,也不受层粘连蛋白受体α6β1抗体的抑制,这表明α7β1是滋养层主要的整合素E8受体。(摘要截断于四百字)

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