体细胞突变
生发中心
美罗华
免疫学
CXCL13型
免疫球蛋白类转换
CXCR5型
医学
B细胞
同型
亲和力成熟
抗体
卵泡期
免疫系统
单克隆抗体
趋化因子
内科学
趋化因子受体
作者
Gaia Mancuso,Tatiana Jofra,Marco Lanzillotta,Alessandro Aiuti,Maria Pia Cicalese,Giulia di Colo,Lorenzo Dagna,Georgia Fousteri,Emanuel Della‐Torre
出处
期刊:Rheumatology
[Oxford University Press]
日期:2021-04-13
卷期号:60 (8): 3947-3949
被引量:13
标识
DOI:10.1093/rheumatology/keab344
摘要
Dear Editor, T-follicular helper (Tfh) cells have been implicated in the pathogenesis of a variety of autoimmune disorders because of their central role in adaptive immune responses [1]. In particular, Tfh cells orchestrate germinal centre reactions by recruiting CXCR5-expressing B-lymphocytes via CXCL13 secretion, and control antigen-dependent maturation, isotype class-switching, and somatic hypermutation of naïve B-cells [1]. IgG4-related disease (IgG4-RD) is an emerging fibro-inflammatory condition characterized by relapsing–remitting tumour-like lesions and increased serum IgG4 concentration [2, 3]. B-lymphocytes play a central pathogenic role in IgG4-RD because active disease is associated with oligoclonal expansion of fibrogenic IgG4+ plasmablasts [4]. In addition, B-cell depletion therapy with rituximab typically leads to rapid clinical improvement and flares occur in parallel with re-emergence of clonally divergent plasmablasts [2–5]. Of note, these B-cell clones are marked by enhanced somatic hypermutation consistent with iterative rounds of...
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