Bijian Krikor, Zhang Linhua, Shen Shi-Hsiang
Mammalian Cell Genetics Group, Biotechnology Research Institute, National Research Council of Canada, 6100 Royalmount av., Montreal, Quebec H4P 2R2, Canada.
Mol Immunol. 2007 Jul;44(15):3682-90. doi: 10.1016/j.molimm.2007.04.005. Epub 2007 May 23.
T cell activation is a critical step in the development of a proper immune response to infection and inflammation. This dynamic process requires efficient T cell receptor signaling, which in turn is modulated by integrin receptor activation and the actin cytoskeleton. CD45 is a key player in T cell receptor mediated signal transduction. However, its exact role in integrin mediated signaling in T cells remains to be elucidated. The present study addresses the relationship between CD45 and beta1-integrin mediated survival signaling in the human T leukemic cell line Jurkat, in which collagen receptors alpha1 beta1 and alpha2 beta1 integrins are localized. Wild type (WT)-Jurkat T cells treated with collagen demonstrated increased cell proliferation and survival. Monitoring the intracellular signaling pathways activated by collagen in WT-Jurkat cells revealed increased focal adhesion kinase (FAK) and extracellular signal-regulated kinase (ERK) activation. Moreover, examination of the actin cytoskeleton of WT-Jurkat T cells treated with collagen demonstrated the presence of an organized cortical actin structure, reminiscent of the survival phenotype. This is in contrast to CD45-deficient J45.01 T cells, where collagen treatment failed to enhance cell proliferation/survival and was unable to stimulate FAK and ERK activity. In addition, the actin cytoskeleton of collagen treated J45.01 T cells was disorganized with cortical actin aggregates present throughout. The importance of an organized actin cytoskeleton to proper cell signaling and survival was further demonstrated by the inability of collagen treated WT-Jurkat cells to activate the FAK and ERK survival pathway in the presence of cytochalasin D, a cytoskeleton-disrupting drug. Consistently, addition of the CD45 specific inhibitor abolished collagen-stimulated FAK and ERK activation in WT-Jurkat cells, further depicting CD45 as the key mediator. Furthermore, collagen-mediated T cell signaling alone was able to activate IL-2 gene transcription devoid of concomitant T cell receptor activation. Taken together, these results are the first to demonstrate that CD45 is important in promoting cell survival by modulating integrin-mediated FAK/ERK signaling in Jurkat T cells and is involved in a distinct signal transduction pathway, separate from T cell receptor signaling, influencing T cell immune responses. Hence, this study will help further our knowledge about beta1-integrin mediated signaling in T cells, which may prove to be essential for the regulation of various T cell mediated immune responses.
T细胞活化是针对感染和炎症产生适当免疫反应过程中的关键步骤。这一动态过程需要高效的T细胞受体信号传导,而T细胞受体信号传导又受到整合素受体活化和肌动蛋白细胞骨架的调节。CD45是T细胞受体介导的信号转导中的关键参与者。然而,其在T细胞整合素介导的信号传导中的确切作用仍有待阐明。本研究探讨了人类T白血病细胞系Jurkat中CD45与β1整合素介导的存活信号之间的关系,在该细胞系中存在胶原蛋白受体α1β1和α2β1整合素。用胶原蛋白处理野生型(WT)-Jurkat T细胞后,细胞增殖和存活增加。监测WT-Jurkat细胞中由胶原蛋白激活的细胞内信号通路,发现粘着斑激酶(FAK)和细胞外信号调节激酶(ERK)的激活增加。此外,对用胶原蛋白处理的WT-Jurkat T细胞的肌动蛋白细胞骨架进行检查,发现存在有组织的皮质肌动蛋白结构,这让人联想到存活表型。这与缺乏CD45的J45.01 T细胞形成对比,在J45.01 T细胞中,胶原蛋白处理未能增强细胞增殖/存活,也无法刺激FAK和ERK活性。此外,用胶原蛋白处理的J45.01 T细胞的肌动蛋白细胞骨架是无序的,整个细胞中都存在皮质肌动蛋白聚集体。在存在细胞松弛素D(一种破坏细胞骨架的药物)的情况下,用胶原蛋白处理的WT-Jurkat细胞无法激活FAK和ERK存活途径,这进一步证明了有组织的肌动蛋白细胞骨架对适当的细胞信号传导和存活的重要性。一致的是,添加CD45特异性抑制剂消除了WT-Jurkat细胞中胶原蛋白刺激的FAK和ERK激活,进一步将CD45描绘为关键介质。此外,单独的胶原蛋白介导的T细胞信号传导能够激活IL-2基因转录,而无需伴随T细胞受体激活。综上所述,这些结果首次证明CD45在通过调节Jurkat T细胞中整合素介导的FAK/ERK信号传导来促进细胞存活方面很重要,并且参与了一条与T细胞受体信号传导不同的独特信号转导途径,影响T细胞免疫反应。因此,本研究将有助于进一步加深我们对T细胞中β1整合素介导的信号传导的了解,这可能被证明对调节各种T细胞介导的免疫反应至关重要。
