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整合素在T细胞归巢至淋巴组织和非淋巴组织部位中的作用:到达并停留于此。

Integrin function in T-cell homing to lymphoid and nonlymphoid sites: getting there and staying there.

作者信息

Denucci Christopher C, Mitchell Jason S, Shimizu Yoji

机构信息

Department of Laboratory Medicine and Pathology, Center for Immunology, Masonic Cancer Center, University of Minnesota Medical School, Minneapolis, MN, USA.

出版信息

Crit Rev Immunol. 2009;29(2):87-109. doi: 10.1615/critrevimmunol.v29.i2.10.

Abstract

The continuous recirculation of naive T cells and their subsequent migration to tissue following activation is crucial for maintaining protective immunity against invading pathogens. The preferential targeting of effector and memory T cells to tissue is instructed during priming and mediated by cell surface expressed adhesion receptors such as integrins. Integrins arc involved in nearly all aspects of T-cell life, including naive T-cell circulation, activation, and finally effector T-cell trafficking and localization. Recent research has revealed that microenvironmental factors present during T-cell priming result in the specific regulation of adhesion/integrin and chemokine receptor expression. Once antigen-experienced T cells enter tissue, further changes in integrin expression may occur that arc critical for T-cell localization, retention, effector function, and survival. This review discusses the function of integrin expression on T cells and the multiple roles integrins play on naive T cells and in directing effector T-cell trafficking to nonlymphoid sites in order to maintain protective adaptive immunity at body barriers.

摘要

初始T细胞的持续再循环及其激活后向组织的迁移对于维持针对入侵病原体的保护性免疫至关重要。效应T细胞和记忆T细胞向组织的优先靶向在启动过程中被指定,并由细胞表面表达的黏附受体(如整合素)介导。整合素几乎参与T细胞生命的各个方面,包括初始T细胞循环、激活,以及最终效应T细胞的运输和定位。最近的研究表明,T细胞启动过程中存在的微环境因素会导致黏附/整合素和趋化因子受体表达的特异性调节。一旦经历抗原的T细胞进入组织,整合素表达可能会发生进一步变化,这对于T细胞的定位、滞留、效应功能和存活至关重要。本综述讨论了整合素在T细胞上表达的功能,以及整合素在初始T细胞上所起的多种作用,以及在引导效应T细胞运输到非淋巴部位以维持机体屏障处的保护性适应性免疫方面所起的作用。

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