Winfield J B, Jarjour W N
Thurston Arthritis Research Center, Division of Rheumatology and Immunology, University of North Carolina, Chapel Hill 27599.
Curr Top Microbiol Immunol. 1991;167:161-89. doi: 10.1007/978-3-642-75875-1_10.
At birth, the immune system is biased toward recognition of microbial antigens in order to protect the host from infection. Recent data suggest that an important initial line of defense in this regard involves autologous stress proteins, especially conserved peptides of hsp60, which are presented to T cells bearing gamma delta receptors by relatively nonpolymorphic class lb molecules. Natural antibodies may represent a parallel B cell mechanism. Through an evolving process of "physiological" autoreactivity and selection by immunodominant stress proteins common to all prokaryotes, B and T cell repertoires expand during life to meet the continuing challenge of infection. Because stress proteins of bacteria are homologous with stress proteins of the host, there exists in genetically susceptible individuals a constant risk of autoimmune disease due to failure of mechanisms for self-nonself discrimination. That stress proteins actually play a role in autoimmune processes is supported by a growing body of evidence which, collectively, suggests that autoreactivity in chronic inflammatory arthritis involves, at least initially, gamma delta cells which recognize epitopes of the stress protein hsp60. Alternate mechanisms for T cell stimulation by stress proteins undoubtedly also exist, e.g., molecular mimicry of the DR beta third hypervariable region susceptibility locus for rheumatoid arthritis by a DnaJ stress protein epitope in gram-negative bacteria. While there still is confusion with respect to the most relevant stress protein epitopes, a central role for stress proteins in the etiology of arthritis appears likely. Furthermore, insight derived from the work thus far in adjuvant-induced arthritis already is stimulating analyses of related phenomena in autoimmune diseases other than those involving joints. Only limited data are available in the area of humoral autoimmunity to stress proteins. Autoantibodies to a number of stress proteins have been identified in SLE and rheumatoid arthritis, but their pathogenetic significance remains to be established. Nevertheless, the capacity of certain stress proteins to bind to multiple proteins in the nucleus and cytoplasm both physiologically and during stress or injury to cells, suggests that stress proteins may be important elements in the "immunogenic particle" concept of the origin of antinuclear and other autoantibodies. In short, this fascinating group of proteins, so mysterious only a few years ago, has impelled truly extraordinary new lines of investigation into the nature of autoimmunity and autoimmune disease.
出生时,免疫系统倾向于识别微生物抗原,以保护宿主免受感染。最近的数据表明,在这方面一个重要的初始防御线涉及自体应激蛋白,尤其是热休克蛋白60(hsp60)的保守肽段,它们由相对非多态性的I类b分子呈递给携带γδ受体的T细胞。天然抗体可能代表一种平行的B细胞机制。通过“生理性”自身反应性以及所有原核生物共有的免疫显性应激蛋白的选择这一不断演变的过程,B细胞和T细胞库在生命过程中不断扩大,以应对持续的感染挑战。由于细菌的应激蛋白与宿主的应激蛋白同源,在遗传易感性个体中,由于自身与非自身识别机制的失效,存在患自身免疫性疾病的持续风险。越来越多的证据支持应激蛋白实际上在自身免疫过程中发挥作用,这些证据共同表明,慢性炎症性关节炎中的自身反应性至少在最初涉及识别应激蛋白hsp60表位的γδ细胞。应激蛋白刺激T细胞的其他机制无疑也存在,例如,革兰氏阴性菌中的DnaJ应激蛋白表位对类风湿关节炎的DRβ第三高变区易感位点的分子模拟。虽然对于最相关的应激蛋白表位仍存在困惑,但应激蛋白在关节炎病因学中似乎起着核心作用。此外,迄今为止从佐剂诱导性关节炎研究中获得的见解已经激发了对除关节疾病外其他自身免疫性疾病相关现象的分析。在体液性自身免疫对应激蛋白的研究领域,仅有有限的数据。在系统性红斑狼疮(SLE)和类风湿关节炎中已鉴定出针对多种应激蛋白的自身抗体,但其致病意义仍有待确定。然而,某些应激蛋白在生理状态下以及细胞应激或损伤期间与细胞核和细胞质中的多种蛋白质结合的能力,表明应激蛋白可能是抗核抗体和其他自身抗体起源的“免疫原性颗粒”概念中的重要元素。简而言之,这组几年前还如此神秘的迷人蛋白质,推动了对自身免疫和自身免疫性疾病本质的真正非凡的新研究方向。
