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一名白癜风患者长期持续存在的黑素细胞特异性CD8 + T细胞中自身抗原识别的分子和功能基础。

Molecular and functional bases of self-antigen recognition in long-term persistent melanocyte-specific CD8+ T cells in one vitiligo patient.

作者信息

Mantovani Stefania, Garbelli Silvia, Palermo Belinda, Campanelli Rita, Brazzelli Valeria, Borroni Giovanni, Martinetti Myriam, Benvenuto Federica, Merlini Giampaolo, della Cuna Gioacchino Robustelli, Rivoltini Licia, Giachino Claudia

机构信息

Experimental Immunology Laboratory, IRCCS Maugeri Foundation, Pavia, Italy.

出版信息

J Invest Dermatol. 2003 Aug;121(2):308-14. doi: 10.1046/j.1523-1747.2003.12368.x.

Abstract

Vitiligo patients possess high frequencies of circulating CD8+ T lymphocytes specific for the melanocyte differentiation antigen Melan-A/MART-1. These self-specific T cells exhibit intact functional properties and their T cell receptors are selected for a narrow range of high affinities of antigen recognition, suggesting their important role in the pathogenesis of vitiligo. In order to understand the molecular base for this unexpected, optimal T cell receptor recognition of a self-antigen, a tetramer-guided ex vivo analysis of the T cell receptor repertoire specific for the Melan-A antigen in a patient affected by vitiligo is reported. All T cell receptors sequenced corresponded to different clonotypes, excluding extensive clonal expansions and revealing a large repertoire of circulating Melan-A-specific T lymphocytes. A certain degree of T cell receptor structural conservation was noticed, however, as a single AV segment contributed to the alpha chain rearrangement in 100% of clones and a conserved amino acid sequence was found in the beta chain complementarity determining region 3 of various high affinity cells. We suggest that the conserved alpha chain confers self-antigen recognition, necessary for intrathymic selection and peripheral homeostasis, to many synonymous T cell receptors, whereas the beta chain fine tunes the T cell receptor affinity of the specific cells. In addition, we demonstrate that many high avidity T cell clones from this patient were capable of specifically lysing normal, HLA-matched melanocytes. These autoreactive clones persisted for more than 3 y in the patient's peripheral blood. These data, together with the skin-homing potential of the clones, directly point to the in vivo pathogenic role of melanocyte-specific cytotoxic T lymphocytes in vitiligo.

摘要

白癜风患者循环中针对黑素细胞分化抗原Melan-A/MART-1的CD8+ T淋巴细胞频率较高。这些自身特异性T细胞表现出完整的功能特性,其T细胞受体针对抗原识别的高亲和力范围进行了狭窄选择,表明它们在白癜风发病机制中起重要作用。为了了解这种对自身抗原意外的、最佳T细胞受体识别的分子基础,本文报道了对一名白癜风患者中针对Melan-A抗原的T细胞受体库进行四聚体引导的体外分析。所有测序的T细胞受体都对应不同的克隆型,排除了广泛的克隆扩增,并揭示了循环中大量Melan-A特异性T淋巴细胞库。然而,注意到一定程度的T细胞受体结构保守性,因为单个AV片段在100%的克隆中促成α链重排,并且在各种高亲和力细胞的β链互补决定区3中发现了保守的氨基酸序列。我们认为,保守的α链赋予许多同义T细胞受体自身抗原识别能力,这对于胸腺内选择和外周稳态是必要的,而β链则微调特定细胞的T细胞受体亲和力。此外,我们证明该患者的许多高亲和力T细胞克隆能够特异性裂解正常的、HLA匹配的黑素细胞。这些自身反应性克隆在患者外周血中持续存在超过3年。这些数据,连同克隆的皮肤归巢潜能,直接指向黑素细胞特异性细胞毒性T淋巴细胞在白癜风中的体内致病作用。

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