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脊柱关节病中HLA - B27免疫失调的一种假说:肠道微生物、B27结构、与B27结合的肽以及趋同进化的作用

A hypothesis for the HLA-B27 immune dysregulation in spondyloarthropathy: contributions from enteric organisms, B27 structure, peptides bound by B27, and convergent evolution.

作者信息

Scofield R H, Warren W L, Koelsch G, Harley J B

机构信息

Oklahoma Medical Research Foundation, Oklahoma City 73104.

出版信息

Proc Natl Acad Sci U S A. 1993 Oct 15;90(20):9330-4. doi: 10.1073/pnas.90.20.9330.

Abstract

Several human rheumatic diseases occur predominantly in persons who carry the histocompatibility (HLA) class I allele B27. They have also been related to Gram-negative enteric microorganisms. In addition, the recent recovery of peptides bound to B27 has allowed an understanding of the structural requirements for their binding. Using the accumulated data base of protein sequences, we have tested a series of hypotheses. First, we have asked whether the primary amino acid sequence of the hypervariable regions of HLA-B27 shares short sequences with the proteins of Gram-negative enteric bacteria. The data demonstrate that, unique among the HLA-B molecules, the hypervariable regions of HLA-B27 unexpectedly share short peptide sequences with proteins from these bacteria. Second, we have asked whether the enteric proteins tend to satisfy the structural requirements for peptide binding to B27 in those regions of the sequence shared with B27. This hypothesis also tends to be true, especially in an allelically variable part of the B27 sequence which is predicted to bind B27 if it were to be presented as a free peptide. We conclude that HLA-B27 and enteric Gram-negative bacteria have undergone a previously unappreciated form of convergent evolution which may be important in the process leading to these rheumatic diseases. Moreover, the regions of the enteric bacterial proteins which are contiguous with the short sequences shared with B27 tend to have structures which are also predicted to bind B27. These observations suggest a mechanism for autoimmunity and lead to the prediction that the B27-associated diseases are mediated by a subset of T-cell receptors, B27, and the peptides bound by B27.

摘要

几种人类风湿性疾病主要发生在携带组织相容性(HLA)I类等位基因B27的人群中。它们也与革兰氏阴性肠道微生物有关。此外,最近对与B27结合的肽段的研究使得人们对其结合的结构要求有了更深入的了解。利用积累的蛋白质序列数据库,我们检验了一系列假设。首先,我们探讨了HLA - B27高变区的一级氨基酸序列是否与革兰氏阴性肠道细菌的蛋白质共享短序列。数据表明,在HLA - B分子中,HLA - B27的高变区出人意料地与这些细菌的蛋白质共享短肽序列。其次,我们研究了肠道蛋白质是否倾向于满足在与B27共享的序列区域中肽与B27结合的结构要求。这一假设似乎也是成立的,特别是在B27序列的一个等位基因可变部分,如果它以游离肽的形式呈现,预计会与B27结合。我们得出结论,HLA - B27和肠道革兰氏阴性细菌经历了一种以前未被认识到的趋同进化形式,这可能在导致这些风湿性疾病的过程中起重要作用。此外,肠道细菌蛋白质中与与B27共享的短序列相邻的区域往往具有也预计会与B27结合的结构。这些观察结果提示了一种自身免疫机制,并导致预测B27相关疾病是由一部分T细胞受体、B27以及与B27结合的肽介导的。

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