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自适应免疫的自我中心功能在免疫反应调节和耐受中的作用。

Self-Centered Function of Adaptive Immunity in Regulation of Immune Responses and in Tolerance.

机构信息

Department of Clinical Microbiology, Polyclinic Breyer, Zagreb, Croatia.

出版信息

J Immunol Res. 2021 Dec 2;2021:7507459. doi: 10.1155/2021/7507459. eCollection 2021.

Abstract

The search for common mechanisms underlying the pathogenesis of chronic inflammatory conditions has crystalized the concept of continuous dual resetting of the immune repertoire (CDR) as a basic principle of the immune system function. Consequently, outlined was the first dynamic comprehensive picture of the immune system function. The goal of this study is to elaborate on regulation of immune responses and mechanisms of tolerance, particularly focusing on adaptive immunity. It is well established that the T/B cell repertoire is selected and maintained based on interactions with self. However, their activation also requires interaction with a self-specific major histocompatibility complex (MHC) "code," i.e., the context of MHC molecules. Therefore, not only repertoire selection and maintenance but also the T/B cell activation and function are self-centered. Thus, adaptive effectors may be primarily focused on the state of self and maintenance of integrity of the self, and only to a certain degree on elimination of the foreign. As examples of such function are used immunologically poorly understood MHC-disparate settings typical for transplantation and pregnancy. Transplantation represents an extreme setting of strong systemic compartment-level adaptive/MHC-restricted immune responses. Described are clinically identified conditions for operational tolerance of MHC-disparate tissues/living systems in allotransplantation, which are in line with the CDR-proposed self-centered regulatory role of T/B cells. In contrast, normal pregnancy is coexistence of semiallogeneic or entirely allogeneic mother and fetus, but without alloreactivity akin to transplantation settings. Presented data support the notion that maintenance of pregnancy is a process that relies predominantly on innate/MHC-independent immune mechanisms. By the inception of hemotrophic stage of pregnancy (second and third trimester), both mother and child are individual living systems, with established adaptive immune repertoires. Although mother-fetus interactions at that point become indirect systemic compartment-level communications, their interactions throughout gestation remain within the innate realm of molecular-level adaptations.

摘要

寻找慢性炎症性疾病发病机制的共同机制,使免疫系统功能的连续双重重置 (CDR) 概念成为一个基本原则。因此,概述了免疫系统功能的第一个动态综合画面。本研究的目的是详细阐述免疫反应的调节和耐受机制,特别是侧重于适应性免疫。众所周知,T/B 细胞库是基于与自身的相互作用而选择和维持的。然而,它们的激活也需要与自身特异性主要组织相容性复合体 (MHC)“代码”,即 MHC 分子的背景相互作用。因此,不仅是库选择和维持,而且 T/B 细胞的激活和功能都是以自我为中心的。因此,适应性效应器可能主要集中在自我状态和自我完整性的维持上,而只是在一定程度上消除外来物。作为这种功能的例子,使用了免疫上理解较差的 MHC 不同设置,这些设置是移植和妊娠的典型特征。移植代表了强烈的全身隔室水平适应性/MHC 受限免疫反应的极端设置。描述了同种异体组织/活体系统在同种异体移植中操作性耐受的临床确定条件,这与 CDR 提出的 T/B 细胞以自我为中心的调节作用一致。相比之下,正常妊娠是半同种异体或完全同种异体的母亲和胎儿共存,但没有类似于移植环境的同种异体反应。所提供的数据支持这样一种观点,即维持妊娠是一个主要依赖于先天/MHC 非依赖性免疫机制的过程。随着妊娠的血液营养阶段(第二和第三个三个月)的开始,母亲和孩子都是独立的活体系统,具有既定的适应性免疫库。尽管此时母亲-胎儿相互作用成为间接的全身隔室水平的交流,但它们在整个妊娠期间的相互作用仍然属于分子水平适应的先天领域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd6a/8692046/66303af092f5/JIR2021-7507459.001.jpg

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