Multimodal repertoire analysis unveils B cell biology in immune-mediated diseases

被引:19
作者
Ota, Mineto [1 ,2 ]
Nakano, Masahiro [1 ,3 ]
Nagafuchi, Yasuo [1 ,2 ]
Kobayashi, Satomi [1 ]
Hatano, Hiroaki [1 ,4 ]
Yoshida, Ryochi [1 ]
Akutsu, Yuko [1 ]
Itamiya, Takahiro [1 ,2 ]
Ban, Nobuhiro [5 ]
Tsuchida, Yumi [1 ]
Shoda, Hirofumi [1 ]
Yamamoto, Kazuhiko [1 ,3 ]
Ishigaki, Kazuyoshi [4 ]
Okamura, Tomohisa [1 ,2 ]
Fujio, Keishi [1 ]
机构
[1] Univ Tokyo, Grad Sch Med, Dept Allergy & Rheumatol, Bunkyo Ku, Tokyo 1138654, Japan
[2] Univ Tokyo, Grad Sch Med, Dept Funct Genom & Immunol Dis, Bunkyo Ku, Tokyo, Japan
[3] RIKEN, Lab Autoimmune Dis, Ctr Integrat Med Sci, Yokohama, Japan
[4] RIKEN, Lab Human Immunogenet, Ctr Integrat Med Sci, Yokohama, Japan
[5] Chugai Pharmaceut Co Ltd, Res Div, Yokohama, Japan
基金
日本科学技术振兴机构;
关键词
B-lymphocytes; lupus erythematosus; systemic; autoimmune diseases; SYSTEMIC-LUPUS-ERYTHEMATOSUS; AUTOREACTIVITY; RESPONSES;
D O I
10.1136/ard-2023-224421
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
ObjectivesDespite the involvement of B cells in the pathogenesis of immune-mediated diseases (IMDs), biological mechanisms underlying their function are scarcely understood. To overcome this gap, here we constructed and investigated a large-scale repertoire catalogue of five B cell subsets of patients with IMDs. MethodsWe mapped B cell receptor regions from RNA sequencing data of sorted B cell subsets. Our dataset consisted of 595 donors under IMDs and health. We characterised the repertoire features from various aspects, including their association with immune cell transcriptomes and clinical features and their response to belimumab treatment. ResultsHeavy-chain complementarity-determining region 3 (CDR-H3) length among naive B cells was shortened among autoimmune diseases. Strong negative correlation between interferon signature strength and CDR-H3 length was observed in naive B cells and suggested the role for interferon in premature B cell development. VDJ gene usage was skewed especially in plasmablasts and unswitched-memory B cells of patients with systemic lupus erythematosus (SLE). We developed a scoring system to quantify this skewing, and it positively correlated with peripheral helper T cell transcriptomic signatures and negatively correlated with the amount of somatic hyper mutations in plasmablasts, suggesting the association of extrafollicular pathway. Further, this skewing led to high usage of IGHV4-34 gene with 9G4 idiotypes in unswitched-memory B cells, which showed a prominent positive correlation with disease activity in SLE. Gene usage skewing in unswitched-memory B cells was ameliorated after belimumab treatment. ConclusionsOur multimodal repertoire analysis enabled us the system-level understanding of B cell abnormality in diseases.
引用
收藏
页码:1455 / 1463
页数:9
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