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T 细胞命运的调控因子:细胞迁移、分化和功能的整合。

Regulators of T-cell fate: Integration of cell migration, differentiation and function.

机构信息

Division of Immunology, Walter and Eliza Hall Institute of Medical Research, Parkville, Victoria, Australia.

Department of Medical Biology, University of Melbourne, Parkville, Victoria, Australia.

出版信息

Immunol Rev. 2019 May;289(1):101-114. doi: 10.1111/imr.12742.

Abstract

A fundamental question in immunology is how cells decide between distinct T helper, effector or memory differentiation fates. These decisions are paramount to overcome infection and establish long-lasting protection. The impact of cell location for the determination of T-cell fate decisions is an emerging field. This review will discuss our current understanding of the migration path that T cells follow, within draining lymph nodes, to steer differentiation down distinct paths of either effector or memory fates. In particular, the regulation of migration and cellular encounters mediated by the chemokine receptor CXCR3 and its ligands will be discussed. The combination of increased antigen density and unique cellular partners play a central role in facilitating the site-specific differentiation of effector T cells, within the interfollicular regions of draining lymph nodes. Recent advances have applied this knowledge to optimize vaccine design to target antigen to lymph nodes. Increased understanding of the regulation of CXCR3 ligands and how T cells integrate multiple chemokine cues will help further progress in this field and allow additional applications to direct cell differentiation outside the lymph node, to enhance memory residency in peripheral tissues and effector anti-tumor responses.

摘要

免疫学中的一个基本问题是细胞如何在不同的 T 辅助、效应或记忆分化命运之间做出选择。这些决策对于克服感染和建立持久的保护至关重要。细胞位置对 T 细胞命运决定的影响是一个新兴领域。本文将讨论我们目前对 T 细胞在引流淋巴结中遵循的迁移途径的理解,以引导其沿着效应或记忆命运的不同途径分化。特别是,将讨论趋化因子受体 CXCR3 及其配体介导的迁移和细胞相互作用的调节。抗原密度的增加和独特的细胞伙伴的组合在促进效应 T 细胞在引流淋巴结的滤泡间区域的特异性分化中起着核心作用。最近的进展将这一知识应用于优化疫苗设计,以将抗原靶向淋巴结。对 CXCR3 配体的调节以及 T 细胞如何整合多种趋化因子线索的理解将有助于该领域的进一步发展,并允许在淋巴结外引导细胞分化,以增强外周组织中的记忆驻留和效应抗肿瘤反应。

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