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针对密切相关的B*2705和B*2703亚型的同种异体反应性T细胞应答的克隆分析。对HLA - B27与脊柱关节病关联的意义。

Clonal analysis of alloreactive T cell responses against the closely related B*2705 and B*2703 subtypes. Implications for HLA-B27 association to spondyloarthropathy.

作者信息

López D, García-Hoyo R, López de Castro J A

机构信息

Center of Molecular Biology Severo Ochoa, Council of Scientific Investigations and Autonomous University of Madrid, Cantoblanco, Spain.

出版信息

J Immunol. 1994 Jun 1;152(11):5557-71.

PMID:8189072
Abstract

Alloreactive responses against closely related HLA-B27 subtypes were compared at the clonal level by fine specificity analysis of anti-B2705 and anti-B2703 CTL clones from unrelated HLA-B27- individuals with target cells expressing B2701 to B2706, and other HLA Ags. T cell epitope sharing between B2705 and other subtypes was B2705 > B2703 > B2702 > B2701 > B2704 > B2706, and correlated with their amino acid differences. This suggests that identical or similar peptides, or peptide motifs, can be presented by multiple HLA-B27 subtypes to T cells, a feature that may be critical for the similar linkage of several subtypes to spondyloarthropathies. Other cross-reactions were predominantly with HLA-B61 and HLA-B60. Marked differences were observed in the nature and frequency of clonal reaction patterns among individuals. They correlated with structural features of the HLA-B Ags from each donor, suggesting that anti-HLA-B27 T cell responses are partially determined by the HLA-B phenotype of the responder. Ability to respond to particular HLA-B27-associated epitopes may determine differences in disease susceptibility among HLA-B27+ individuals. The anti-B2703 and anti-B2705 responses in the same individual were different. A major feature of anti-B2703 CTL was that a large majority cross-reacted with B2705. This can be explained by the effect of the single amino acid change in B2703 on peptide binding and suggests that the B2703-bound peptide repertoire is mainly a subset of that bound to B2705, with few peptides being specifically presented by B*2703 to T cells.

摘要

通过对来自无关的HLA - B27阴性个体的抗B2705和抗B2703细胞毒性T淋巴细胞(CTL)克隆与表达B2701至B2706及其他HLA抗原的靶细胞进行精细特异性分析,在克隆水平上比较了针对密切相关的HLA - B27亚型的同种异体反应。B2705与其他亚型之间的T细胞表位共享情况为B2705 > B2703 > B2702 > B2701 > B2704 > B2706,且与它们的氨基酸差异相关。这表明多个HLA - B27亚型可将相同或相似的肽段或肽基序呈递给T细胞,这一特征可能对于几种亚型与脊柱关节病的相似关联至关重要。其他交叉反应主要发生在HLA - B61和HLA - B60之间。在个体间克隆反应模式的性质和频率上观察到显著差异。它们与每个供体的HLA - B抗原的结构特征相关,表明抗HLA - B27 T细胞反应部分由应答者的HLA - B表型决定。对特定HLA - B27相关表位的应答能力可能决定HLA - B27阳性个体之间疾病易感性的差异。同一个体中的抗B2703和抗B2705反应不同。抗B2703 CTL的一个主要特征是绝大多数与B2705发生交叉反应。这可以通过B2703中单个氨基酸变化对肽结合的影响来解释,表明与B2703结合的肽库主要是与B2705结合的肽库的一个子集,很少有肽段由B*2703特异性呈递给T细胞。

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