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化学转化的人类细胞中整合素受体表达的改变:层粘连蛋白和胶原蛋白受体复合物的特异性增强。

Alterations in integrin receptor expression on chemically transformed human cells: specific enhancement of laminin and collagen receptor complexes.

作者信息

Dedhar S, Saulnier R

机构信息

Department of Advanced Therapeutics, Cancer Control Agency of British Columbia, Vancouver, Canada.

出版信息

J Cell Biol. 1990 Feb;110(2):481-9. doi: 10.1083/jcb.110.2.481.

Abstract

The abilities of malignant tumor cells to bind and migrate through basement membranes are important steps in invasion and metastasis. Malignant tumor cells would therefore be expected to express receptors on their surfaces for basement membrane and stromal components, such as collagens, laminin, and fibronectin, although the pattern of expression of these receptors on the malignant cells may be different from that on their normal progenitors. We report here that chemically transformed tumorigenic human cells express an altered pattern of integrin receptors on their cell surfaces as compared with their untransformed nontumorigenic counterparts. Specifically, N-methyl-N'-nitro-N-nitrosoguanidine transformation of HOS cells into highly tumorigenic cells results in a significant specific increase in the expression of (in descending order of level of cell surface expression) the integrins alpha 6/beta 1, alpha 2/beta 1, and alpha 1/beta 1, which are receptors for laminin, collagens, and collagen type IV and laminin, respectively. The level of expression of two fibronectin receptor integrins, alpha 5/beta 1 and alpha 3/beta 1, are, however, unaltered, whereas the level of expression of vitronectin receptor integrin, alpha v/beta 3, is drastically reduced on the transformed cells. Consistent with the increased expression of laminin and collagen receptors and the decreased expression of vitronectin receptors on the transformed cells, these cells attached three- to fivefold more strongly to laminin and collagen but attached very poorly to vitronectin. The MNNG-HOS cells were also found to have a greater potential for invasion through reconstituted basement membrane, matrigel, the major components of which are laminin and type IV collagen. The invasion of both the HOS and MNNG-HOS cells was inhibited 45-50% by a polyclonal anti-fibronectin receptor antibody. However, although the invasion of HOS cells could be inhibited up to 75% by an anti-alpha 6 monoclonal antibody, a similar concentration of this antibody had no effect on the alpha 6-overproducing MNNG-HOS cells. A fivefold higher concentration of this antibody did result in partial inhibition of MNNG-HOS invasion. These data indicate a critical role for the alpha 6/beta 1 laminin receptor in the invasion of these cells through basement membranes and demonstrate that chemical transformation of nontumorigenic human cells to highly tumorigenic cells is associated with an altered pattern of integrin expression which may play a direct role in the increased capacity of these cells to bind and invade through basement membranes.

摘要

恶性肿瘤细胞黏附并穿过基底膜的能力是侵袭和转移过程中的重要步骤。因此,恶性肿瘤细胞表面可能会表达针对基底膜和基质成分(如胶原蛋白、层粘连蛋白和纤连蛋白)的受体,尽管这些受体在恶性细胞上的表达模式可能与其正常祖细胞不同。我们在此报告,与未转化的非致瘤性人类细胞相比,化学转化的致瘤性人类细胞在其细胞表面表达的整合素受体模式发生了改变。具体而言,将HOS细胞用N-甲基-N'-硝基-N-亚硝基胍转化为高致瘤性细胞后,(按细胞表面表达水平从高到低排列)整合素α6/β1、α2/β1和α1/β1的表达显著特异性增加,它们分别是层粘连蛋白、胶原蛋白以及IV型胶原蛋白和层粘连蛋白的受体。然而,两种纤连蛋白受体整合素α5/β1和α3/β1的表达水平未改变,而玻连蛋白受体整合素αv/β3在转化细胞上的表达水平则大幅降低。与转化细胞上层粘连蛋白和胶原蛋白受体表达增加以及玻连蛋白受体表达减少一致,这些细胞与层粘连蛋白和胶原蛋白的附着能力增强了三到五倍,但与玻连蛋白的附着能力很差。还发现MNNG-HOS细胞通过重组基底膜基质胶(其主要成分是层粘连蛋白和IV型胶原蛋白)进行侵袭的潜力更大。多克隆抗纤连蛋白受体抗体可使HOS细胞和MNNG-HOS细胞的侵袭能力均受到45%-50%的抑制。然而,尽管抗α6单克隆抗体可使HOS细胞的侵袭能力受到高达75%的抑制,但相同浓度的该抗体对α6过量表达的MNNG-HOS细胞却没有作用。五倍高浓度的该抗体确实导致MNNG-HOS细胞的侵袭受到部分抑制。这些数据表明α6/β1层粘连蛋白受体在这些细胞穿过基底膜的侵袭过程中起关键作用,并证明非致瘤性人类细胞向高致瘤性细胞的化学转化与整合素表达模式的改变有关,这可能在这些细胞与基底膜结合及侵袭能力增强中起直接作用。

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