T细胞受体
CD8型
免疫学
发病机制
强直性脊柱炎
医学
抗原
人类白细胞抗原
表型
T细胞
生物
免疫系统
遗传学
基因
作者
Ekaterina A. Komech,Mikhail V. Pogorelyy,Evgeniy S. Egorov,Olga V. Britanova,Denis V. Rebrikov,А Г Бочкова,Е. Шмидт,Nadejda A. Shostak,Mikhail Shugay,Sergey Lukyanov,Ilgar Z. Mamedov,Yuri B. Lebedev,Dmitriy M. Chudakov,Ivan V. Zvyagin
出处
期刊:Rheumatology
[Oxford University Press]
日期:2018-01-22
卷期号:57 (6): 1097-1104
被引量:49
标识
DOI:10.1093/rheumatology/kex517
摘要
The risk of AS is associated with genomic variants related to antigen presentation and specific cytokine signalling pathways, suggesting the involvement of cellular immunity in disease initiation/progression. The aim of the present study was to explore the repertoire of TCR sequences in healthy donors and AS patients to uncover AS-linked TCR variants. Using quantitative molecular-barcoded 5′-RACE, we performed deep TCR β repertoire profiling of peripheral blood (PB) and SF samples for 25 AS patients and 108 healthy donors. AS-linked TCR variants were identified using a new computational approach that relies on a probabilistic model of the VDJ rearrangement process. Using the donor-agnostic probabilistic model, we reveal a TCR β motif characteristic for PB of AS patients, represented by eight highly homologous amino acid sequence variants. Some of these variants were previously reported in SF and PB of patients with ReA and in PB of AS patients. We demonstrate that identified AS-linked clones have a CD8+ phenotype, present at relatively low frequencies in PB, and are significantly enriched in matched SF samples of AS patients. Our results suggest the involvement of a particular antigen-specific subset of CD8+ T cells in AS pathogenesis, confirming and expanding earlier findings. The high similarity of the clonotypes with the ones found in ReA implies common mechanisms for the initiation of the diseases.
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