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细菌β1整合素配体侵袭素对静息人T细胞的极晚期抗原4依赖性黏附及共刺激作用。

Very late antigen 4-dependent adhesion and costimulation of resting human T cells by the bacterial beta 1 integrin ligand invasin.

作者信息

Ennis E, Isberg R R, Shimizu Y

机构信息

Department of Microbiology and Immunology, University of Michigan Medical School, Ann Arbor 48109.

出版信息

J Exp Med. 1993 Jan 1;177(1):207-12. doi: 10.1084/jem.177.1.207.

Abstract

Bacteria and viruses often use the normal biological properties of host adhesion molecules to infect relevant host cells. The outer membrane bacterial protein invasin mediates the attachment of Yersinia pseudotuberculosis to human cells. In vitro studies have shown that four members of the very late antigen (VLA) integrin family of adhesion molecules, VLA-3, VLA-4, VLA-5, and VLA-6, can bind to invasin. Since CD4+ T cells express and use these integrins, we have investigated the interaction of CD4+ T cells with purified invasin. Although VLA integrin-mediated adhesion of T cells to other ligands such as fibronectin does not occur at high levels unless the T cells are activated, resting T cells bind strongly to purified invasin. The binding of resting T cells to invasin requires metabolic activity and an intact cytoskeleton. Although CD4+ T cells express VLA-3, VLA-4, VLA-5, and VLA-6, monoclonal antibody (mAb) blocking studies implicate only VLA-4 as a T cell invasin receptor. Like other integrin ligands, invasin can facilitate T cell proliferative responses induced by a CD3-specific mAb. These results suggest that the nature of the integrin ligand is a critical additional factor that regulates T cell integrin activity, and that direct interactions of T cells with bacterial pathogens such as Yersinia may be relevant to host immune responses to bacterial infection.

摘要

细菌和病毒常常利用宿主黏附分子的正常生物学特性来感染相关宿主细胞。外膜细菌蛋白侵袭素介导假结核耶尔森菌与人细胞的附着。体外研究表明,黏附分子极晚期抗原(VLA)整合素家族的四个成员,即VLA - 3、VLA - 4、VLA - 5和VLA - 6,能够与侵袭素结合。由于CD4⁺T细胞表达并利用这些整合素,我们研究了CD4⁺T细胞与纯化侵袭素的相互作用。尽管除非T细胞被激活,否则VLA整合素介导的T细胞与其他配体(如纤连蛋白)的黏附水平不高,但静息T细胞能与纯化的侵袭素强烈结合。静息T细胞与侵袭素的结合需要代谢活性和完整的细胞骨架。虽然CD4⁺T细胞表达VLA - 3、VLA - 4、VLA - 5和VLA - 6,但单克隆抗体(mAb)阻断研究表明只有VLA - 4作为T细胞侵袭素受体。与其他整合素配体一样,侵袭素能够促进由CD3特异性mAb诱导的T细胞增殖反应。这些结果表明,整合素配体的性质是调节T细胞整合素活性的一个关键附加因素,并且T细胞与诸如耶尔森菌等细菌病原体的直接相互作用可能与宿主对细菌感染的免疫反应相关。

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