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αvβ5整合素受体调节玻连蛋白的受体介导内吞作用。

The alpha v beta 5 integrin receptor regulates receptor-mediated endocytosis of vitronectin.

作者信息

Panetti T S, McKeown-Longo P J

机构信息

Department of Physiology and Cell Biology, Albany Medical College, New York 12208.

出版信息

J Biol Chem. 1993 Jun 5;268(16):11492-5.

PMID:7685013
Abstract

Vitronectin is an adhesive glycoprotein that binds to the extracellular matrix and interacts with integrin receptors on the surface of adherent cells. Previous studies have demonstrated that the conformationally altered, heparin binding form of vitronectin is removed from the matrix by receptor-mediated endocytosis and degraded through a lysosomal pathway (Panetti, T. S., and McKeown-Longo, P. J. (1993) J. Biol. Chem. 268, 11988-11993). The present studies were undertaken to determine the role of cell surface integrins in the endocytosis and degradation of vitronectin. RGDS peptides, used to disrupt the binding of vitronectin to cell surface integrins, inhibited degradation of vitronectin but had no effect on the binding of vitronectin to the cell layer. Localization of vitronectin in the cell layer by indirect immunofluorescence indicated that the RGDS peptides inhibited degradation by preventing the internalization of vitronectin by the cells. To determine which vitronectin receptor was involved in mediating the endocytosis, vitronectin degradation was measured in the presence of monoclonal antibodies. Antibodies against the alpha v beta 5 but not the alpha v beta 3 integrin inhibited degradation of vitronectin by 80%. This study demonstrates a new role for integrins in regulating internalization and degradation of molecules from the extracellular matrix.

摘要

玻连蛋白是一种黏附糖蛋白,它可与细胞外基质结合,并与黏附细胞表面的整合素受体相互作用。先前的研究表明,构象改变的、与肝素结合的玻连蛋白形式通过受体介导的内吞作用从基质中清除,并通过溶酶体途径降解(帕内蒂,T. S.,和麦基翁 - 隆戈,P. J.(1993年)《生物化学杂志》268卷,11988 - 11993页)。本研究旨在确定细胞表面整合素在玻连蛋白的内吞作用和降解过程中的作用。用于破坏玻连蛋白与细胞表面整合素结合的RGDS肽可抑制玻连蛋白的降解,但对玻连蛋白与细胞层的结合没有影响。通过间接免疫荧光对玻连蛋白在细胞层中的定位表明,RGDS肽通过阻止细胞对玻连蛋白的内化来抑制降解。为了确定哪种玻连蛋白受体参与介导内吞作用,在存在单克隆抗体的情况下测量玻连蛋白的降解。抗αvβ5整合素而非抗αvβ3整合素的抗体可抑制80%的玻连蛋白降解。这项研究证明了整合素在调节细胞外基质分子的内化和降解方面的新作用。

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