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由整合素α4β1介导的CCL25刺激的T细胞黏附所需的细胞内信号传导。

Intracellular signaling required for CCL25-stimulated T cell adhesion mediated by the integrin alpha4beta1.

作者信息

Parmo-Cabañas Marisa, García-Bernal David, García-Verdugo Rosa, Kremer Leonor, Márquez Gabriel, Teixidó Joaquin

机构信息

Department of Molecular and Cellular Physiopathology, Centro de Investigaciones Biológicas (CSIC), Madrid, Spain.

出版信息

J Leukoc Biol. 2007 Aug;82(2):380-91. doi: 10.1189/jlb.1206726. Epub 2007 May 17.

DOI:10.1189/jlb.1206726
PMID:17510295
Abstract

The alpha4beta1 integrin is expressed on thymocytes and mediates cell attachment to its ligands CS-1/fibronectin (CS-1/FN) and VCAM-1 in the thymus. The chemokine CCL25 is highly expressed in the thymus, where it binds to its receptor CCR9 on thymocytes promoting migration and activation. We show here that alpha4beta1 and CCR9 are coexpressed mainly on double- and single-positive thymocytes and that CCL25 strongly stimulates CD4(+)CD8(+) and CD4(+)CD8(-) adhesion to CS-1/FN and VCAM-1. CCL25 rapidly activated the GTPases Rac and Rap1 on thymocytes, and this activation was required for stimulation of adhesion, as detected using the CCR9(+)/alpha4beta1(+) human T cell line Molt-4. To study the role on CCL25-stimulated adhesion of the Rac downstream effector Wiskott-Aldrich syndrome protein family verproline-homologous protein 2 (WAVE2) as well as of Rap1-GTP-interacting proteins, regulator of adhesion and cell polarization enriched in lymphoid tissues (RAPL) and Rap1-GTP-interacting adapter molecule (RIAM), we knocked down their expression and tested transfectant attachment to alpha4beta1 ligands. We found that WAVE2 and RAPL but not RIAM were required for efficient triggering by CCL25 of T cell adhesion to CS-1/FN and VCAM-1. Although Rac and Rap1 activation was required during early steps of T cell adhesion stimulated by CCL25, WAVE2 was needed for the development of actin-dependent T cell spreading subsequent to adhesion strengthening but not during initial alpha4beta1-ligand interactions. These results suggest that regulation by CCL25 of adhesion of thymocyte subpopulations mediated by alpha4beta1 could contribute to control their trafficking in the thymus during maturation, and identify Rac-WAVE2 and Rap1-RAPL as pathways whose activation is required in inside-out signaling, leading to stimulated adhesion.

摘要

α4β1整合素在胸腺细胞上表达,并介导细胞与胸腺中其配体CS-1/纤连蛋白(CS-1/FN)和血管细胞黏附分子-1(VCAM-1)的附着。趋化因子CCL25在胸腺中高表达,它在胸腺中与胸腺细胞上的受体CCR9结合,促进迁移和激活。我们在此表明,α4β1和CCR9主要在双阳性和单阳性胸腺细胞上共表达,并且CCL25强烈刺激CD4(+)CD8(+)和CD4(+)CD8(-)细胞与CS-1/FN和VCAM-1的黏附。CCL25迅速激活胸腺细胞上的GTP酶Rac和Rap1,并且如使用CCR9(+)/α4β1(+)人T细胞系Molt-4所检测到的,这种激活是刺激黏附所必需的。为了研究Rac下游效应器威斯科特-奥尔德里奇综合征蛋白家族维甲酸同源蛋白2(WAVE2)以及Rap1-GTP相互作用蛋白、富含淋巴组织的黏附与细胞极化调节因子(RAPL)和Rap1-GTP相互作用衔接分子(RIAM)在CCL25刺激的黏附中的作用,我们敲低它们的表达并测试转染子与α4β1配体的附着。我们发现,WAVE2和RAPL而非RIAM是CCL25有效触发T细胞与CS-1/FN和VCAM-1黏附所必需的。尽管在CCL25刺激的T细胞黏附早期步骤中需要Rac和Rap1激活,但在黏附增强后肌动蛋白依赖性T细胞铺展的发展中需要WAVE2,而在最初的α4β1-配体相互作用期间则不需要。这些结果表明,CCL25对由α4β1介导的胸腺细胞亚群黏附的调节可能有助于在成熟过程中控制它们在胸腺中的运输,并确定Rac-WAVE2和Rap1-RAPL为在内向外信号传导中其激活是刺激黏附所必需的途径。

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