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重症肌无力患者人类乙酰胆碱受体α亚基上的CD4 + T细胞表位谱:一项合成肽研究

CD4+ T-epitope repertoire on the human acetylcholine receptor alpha subunit in severe myasthenia gravis: a study with synthetic peptides.

作者信息

Manfredi A A, Protti M P, Wu X D, Howard J F, Conti-Tronconi B M

机构信息

Department of Biochemistry, College of Biological Sciences, University of Minnesota, St. Paul 55108.

出版信息

Neurology. 1992 May;42(5):1092-100. doi: 10.1212/wnl.42.5.1092.

Abstract

The alpha subunit of the nicotinic acetylcholine receptor (AChR) seems crucial in the pathogenesis of the autoimmune paralysis myasthenia gravis (MG) because it contains both the epitopes that dominate the antibody response against the AChR and those recognized by CD4+ AChR-specific T helper (Th) cells. To define the repertoire of anti-AChR Th cells, we investigated the response of unselected blood CD4+ cells or total lymphocytes, or both, from 22 MG patients to 20-residue overlapping synthetic peptides, screening the complete sequence of human-muscle AChR alpha subunit. Several epitopes were identified. Only the most severely affected patients recognized alpha subunit epitopes, and they were mainly young women. Detection of in vitro AChR-specific CD4+ response was facilitated by removal of the CD8+ cells because in two patients a clear response to several alpha subunit peptide sequences could be detected when CD(8+)-depleted cells were used, while their total peripheral blood mononuclear cell population did not respond to any alpha subunit peptide. Although each patient had a unique pattern of peptide recognition, four immunodominant regions recognized by long-term AChR-specific CD4+ T-cell lines, or flanking peptide sequences, were recognized most frequently (residues 48-67, 101-137, 293-337, and 308-437).

摘要

烟碱型乙酰胆碱受体(AChR)的α亚基似乎在自身免疫性麻痹性重症肌无力(MG)的发病机制中起关键作用,因为它既包含主导针对AChR抗体反应的表位,也包含被CD4⁺ AChR特异性辅助性T(Th)细胞识别的表位。为了确定抗AChR Th细胞的组成,我们研究了22例MG患者未分选的血液CD4⁺细胞或全淋巴细胞或两者对20个残基重叠合成肽的反应,筛选了人肌肉AChR α亚基的完整序列。确定了几个表位。只有受影响最严重的患者识别α亚基表位,且他们主要是年轻女性。去除CD8⁺细胞有助于检测体外AChR特异性CD4⁺反应,因为在两名患者中,当使用去除CD8⁺的细胞时,可以检测到对几个α亚基肽序列的明确反应,而其外周血单个核细胞总体对任何α亚基肽均无反应。尽管每位患者都有独特的肽识别模式,但长期AChR特异性CD4⁺ T细胞系识别的四个免疫显性区域或侧翼肽序列被识别的频率最高(第48 - 67位、101 - 137位、293 - 337位和308 - 437位残基)。

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