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主要组织相容性复合体I类分子与抗细胞内病原体的能力

Major histocompatibility complex class I molecules and resistance against intracellular pathogens.

作者信息

Ojcius D M, Delarbre C, Kourilsky P, Gachelin G

机构信息

Institut Pasteur, Unité de Biologie Moléculaire du Gène, Paris, France.

出版信息

Crit Rev Immunol. 1994;14(3-4):193-220. doi: 10.1615/critrevimmunol.v14.i3-4.10.

DOI:10.1615/critrevimmunol.v14.i3-4.10
PMID:7755874
Abstract

The immune system employs a temporal hierarchy of effector mechanisms to combat infections by intracellular pathogens. The nonspecific response is independent of MHC and can be activated rapidly, while the specific response is slower, more specific, and requires major histocompatibility complex (MHC) molecules. MHC-dependent responses have been characterized extensively in vitro for antigens presented by polymorphic MHC class Ia and class II proteins and recognized by T lymphocytes carrying alpha/beta T-cell receptors (TcR). Growing indirect evidence has implicated monomorphic MHC class Ib proteins and gamma/delta T lymphocytes in defense against bacterial infections, but the biochemical and immunological behavior of class Ib proteins and gamma/delta TcR has not been well characterized, and most hypotheses involving these proteins have relied on data obtained with polymorphic MHC proteins and alpha/beta TcR. An overview of studies describing bacterial infections in vivo suggests that, in many cases, MHC class I-dependent effector cells may not be indispensable for effective immune responses, exerting instead a modulatory effect during the course of infection. Furthermore, many class Ib proteins have probably specialized to present stress antigens and conserved microbial antigens, which may be recognized by gamma/delta T cells through an interaction that is qualitatively very different from alpha/beta TcR binding to class I and class II proteins.

摘要

免疫系统利用效应机制的时间层次结构来对抗细胞内病原体的感染。非特异性反应独立于主要组织相容性复合体(MHC),可以迅速激活,而特异性反应则较慢、更具特异性,并且需要主要组织相容性复合体(MHC)分子。对于由多态性MHC Ia类和II类蛋白呈递并被携带α/β T细胞受体(TcR)的T淋巴细胞识别的抗原,MHC依赖性反应已在体外得到广泛表征。越来越多的间接证据表明,单态性MHC Ib类蛋白和γ/δ T淋巴细胞参与了对细菌感染的防御,但Ib类蛋白和γ/δ TcR的生化和免疫行为尚未得到很好的表征,并且大多数涉及这些蛋白的假说都依赖于用多态性MHC蛋白和α/β TcR获得的数据。对描述体内细菌感染的研究的概述表明,在许多情况下,MHC I类依赖性效应细胞对于有效的免疫反应可能不是必不可少的,而是在感染过程中发挥调节作用。此外,许多Ib类蛋白可能专门呈递应激抗原和保守的微生物抗原,γ/δ T细胞可能通过一种与α/β TcR与I类和II类蛋白结合在性质上非常不同的相互作用来识别这些抗原。

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