Lowin-Kropf B, Shapiro V S, Weiss A
Department of Medicine, University of California, San Francisco, San Francisco, California 94143, USA.
J Cell Biol. 1998 Feb 23;140(4):861-71. doi: 10.1083/jcb.140.4.861.
Binding of a T cell to an appropriate antigen-presenting cell (APC) induces the rapid reorientation of the T cell cytoskeleton and secretory apparatus towards the cell-cell contact site in a T cell antigen receptor (TCR) and peptide/major histocompatibility complex-dependent process. Such T cell polarization directs the delivery of cytokines and cytotoxic mediators towards the APC and contributes to the highly selective and specific action of effector T cells. To study the signaling pathways that regulate cytoskeletal rearrangements in T lymphocytes, we set up a conjugate formation assay using Jurkat T cells as effectors and cell-sized latex beads coated with various antibodies as artificial APCs. Here, we report that beads coated with antibodies specific for the TCR-CD3 complex were sufficient to induce T cell polarization towards the bead attachment site, as judged by reorientation of the microtubule-organizing center (MTOC) and localized actin polymerization. Thus, these cytoskeletal changes did not depend on activation of additional coreceptors. Moreover, single subunits of the TCR complex, namely TCR-zeta and CD3epsilon, were equally effective in inducing cytoskeletal polarization. However, mutagenesis of the immunoreceptor tyrosine-based activation motifs (ITAMs), present three times in TCR-zeta and once in CD3epsilon, revealed that the induction of cytoskeletal rearrangements required the presence of at least one intact ITAM. In agreement with this result, lack of functional Lck, the protein tyrosine kinase responsible for ITAM phosphorylation, abolished both MTOC reorientation and polarized actin polymerization. Both inhibitor and transient overexpression studies demonstrated that MTOC reorientation could occur in the absence of Ras activation. Our results suggest that APC-induced T cell polarization is a TCR-mediated event that is coupled to the TCR by the same signaling motif as TCR-induced gene activation, but diverges in its distal signaling requirements.
T细胞与合适的抗原呈递细胞(APC)结合,会在T细胞抗原受体(TCR)和肽/主要组织相容性复合体依赖性过程中,诱导T细胞细胞骨架和分泌装置迅速重新定向至细胞间接触部位。这种T细胞极化将细胞因子和细胞毒性介质导向APC,并有助于效应T细胞高度选择性和特异性的作用。为了研究调节T淋巴细胞细胞骨架重排的信号通路,我们建立了一种共轭形成试验,使用Jurkat T细胞作为效应细胞,并用包被有各种抗体的细胞大小的乳胶珠作为人工APC。在此,我们报告,包被有TCR-CD3复合体特异性抗体的珠子足以诱导T细胞向珠子附着部位极化,这可通过微管组织中心(MTOC)的重新定向和局部肌动蛋白聚合来判断。因此,这些细胞骨架变化不依赖于其他共受体的激活。此外,TCR复合体的单个亚基,即TCR-ζ和CD3ε,在诱导细胞骨架极化方面同样有效。然而,对TCR-ζ中出现三次且CD3ε中出现一次的基于免疫受体酪氨酸的激活基序(ITAM)进行诱变后发现,细胞骨架重排的诱导需要至少一个完整的ITAM存在。与该结果一致,缺乏负责ITAM磷酸化的蛋白酪氨酸激酶Lck,会消除MTOC重新定向和极化肌动蛋白聚合。抑制剂和瞬时过表达研究均表明,在没有Ras激活的情况下也可发生MTOC重新定向。我们的结果表明,APC诱导的T细胞极化是一个TCR介导的事件,它通过与TCR诱导基因激活相同的信号基序与TCR偶联,但在其远端信号需求上有所不同。
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