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T细胞活化与细胞骨架:二者缺一不可。

T cell activation and the cytoskeleton: you can't have one without the other.

作者信息

Gomez Timothy S, Billadeau Daniel D

机构信息

Department of Immunology and Oncology Research, College of Medicine, Mayo Clinic, Rochester, MN 55905, USA.

出版信息

Adv Immunol. 2008;97:1-64. doi: 10.1016/S0065-2776(08)00001-1.

DOI:10.1016/S0065-2776(08)00001-1
PMID:18501768
Abstract

More than a quarter of a century has passed since the observation that T cells rapidly polarize their actin and microtubule cytoskeletal systems toward antigen-presenting cells during activation. Since this initial discovery, several receptors on T cells (e.g., T cell receptor [TCR], co-receptors, integrins, and chemokine receptors) have been identified to regulate these two cytoskeletal networks through complex signaling pathways, which are still being elucidated. There is now an undeniable body of biochemical, pharmacological, and genetic evidence indicating that regulators of actin and microtubule dynamics are crucial for T cell activation and effector functions. In fact, the actin cytoskeleton participates in the initial clustering of TCR-major histocompatibility complex or peptide complexes, formation and stabilization of the immune synapse, integrin-mediated adhesion, and receptor sequestration, whereas both the actin and microtubule cytoskeletons regulate the establishment of cell polarity, cell migration, and directed secretion of cytokines and cytolytic granules. Over the past several years, we have begun to more thoroughly understand the contributions of specific actin-regulatory and actin-nucleating proteins that govern these processes. Herein, we discuss our current understanding of how activating receptors on T lymphocytes regulate the actin and microtubule cytoskeletons, and how in turn, these distinct but integrated cytoskeletal networks coordinate T cell immune responses.

摘要

自观察到T细胞在激活过程中迅速将其肌动蛋白和微管细胞骨架系统朝着抗原呈递细胞极化以来,已经过去了25年多。自这一最初发现以来,T细胞上的几种受体(如T细胞受体[TCR]、共受体、整合素和趋化因子受体)已被确定通过复杂的信号通路调节这两个细胞骨架网络,而这些信号通路仍在研究之中。现在,有大量不可否认的生化、药理学和遗传学证据表明,肌动蛋白和微管动力学的调节因子对T细胞激活和效应功能至关重要。事实上,肌动蛋白细胞骨架参与TCR-主要组织相容性复合体或肽复合体的初始聚集、免疫突触的形成和稳定、整合素介导的黏附以及受体隔离,而肌动蛋白和微管细胞骨架都调节细胞极性的建立、细胞迁移以及细胞因子和溶细胞颗粒的定向分泌。在过去几年里,我们开始更全面地了解特定的肌动蛋白调节蛋白和肌动蛋白成核蛋白在这些过程中的作用。在此,我们讨论目前对T淋巴细胞上的激活受体如何调节肌动蛋白和微管细胞骨架,以及反过来,这些不同但相互整合的细胞骨架网络如何协调T细胞免疫反应的理解。

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