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Circulating Follicular Helper–Like T Cells in Systemic Lupus Erythematosus: Association With Disease Activity

CXCR5型 免疫学 CD38 免疫球蛋白D CD19 医学 流式细胞术 抗体 B细胞 生物 生发中心 干细胞 川地34 遗传学
作者
Jin‐Young Choi,John Hsi‐en Ho,Sandra Gofinet Pasoto,Viviane Bunin,Sang Taek Kim,Solange Carrasco,Eduardo Ferreira Borba,Célio Roberto Gonçalves,Priscila Ribas de Farias Costa,Esper G. Kallás,Eloísa Bonfá,Joseph Craft
出处
期刊:Arthritis & rheumatology [Wiley]
卷期号:67 (4): 988-999 被引量:276
标识
DOI:10.1002/art.39020
摘要

Objective To assess circulating follicular helper T (Tfh)–like CD4+ T cells in patients with systemic lupus erythematosus (SLE) and determine their relationship to disease activity. Methods Blood samples from patients with SLE, as well as blood samples from patients with Behçet's disease (BD) and healthy individuals as controls, were analyzed. In all samples, circulating Tfh‐like cells were enumerated by flow cytometry, using, as markers, expression of CXCR5, inducible T cell costimulator (ICOS), and programmed death 1 (PD‐1) protein, as well as secretion of interleukin‐21 (IL‐21). The frequency of circulating Tfh‐like cells was compared to that of circulating plasmablasts (CD19+IgD−CD38+). In addition, the possible association of circulating Tfh‐like cells with the SLE Disease Activity Index (SLEDAI) was evaluated. Results The subset of circulating Tfh‐like T cells, identified as CXCR5 high ICOS high PD‐1 high , was expanded in the blood of SLE patients compared to controls. Circulating Tfh‐like cells were found to produce IL‐21 and had lower expression of CCR7 as compared to that in circulating CXCR5 high central memory T cells, thereby enabling their distinction. Expression of PD‐1, but not ICOS or CXCR5, was significantly elevated in circulating Tfh‐like cells from SLE patients compared to controls. PD‐1 expression among CXCR5 high circulating Tfh‐like cells correlated with the SLEDAI, frequency of circulating plasmablasts, and anti–double‐stranded DNA antibody positivity, but not with disease duration or past organ injury; rather, this cell profile appeared to be a reflection of current active disease. Conclusion Circulating Tfh‐like cells are associated with disease activity in SLE, suggesting that their presence indicates abnormal homeostasis of T cell–B cell collaboration, with a causal relationship that is central to disease pathogenesis. These findings also suggest that circulating Tfh‐like cells provide a surrogate for aberrant germinal center activity in SLE, and that their PD‐1 expression offers a tool for measuring disease activity and monitoring the response to therapies.
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