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Alterations in exhausted and classical memory B cells in lupus nephritis – Relationship with disease relapse

狼疮性肾炎 免疫学 系统性红斑狼疮 医学 疾病 肾炎 内科学
作者
Litong Zhu,Yick Hei Wong,Sunny S.H. Wong,Chi Yuen Cheung,Jason K.H. Sher,Irene Yam,Susan Yung,Tak Mao Chan,Desmond Y. H. Yap
出处
期刊:Clinical Immunology [Elsevier]
卷期号:265: 110284-110284
标识
DOI:10.1016/j.clim.2024.110284
摘要

B cell exhaustion is a functional abnormality of B lymphocytes observed in chronic infections and shows association with autoreactivity. The role of exhausted and classical memory B cells in maintaining disease stability of lupus nephritis (LN) remains unclear. We measured classical memory (CD19+CD21+CD27+), exhausted B cells (CD19+CD21−CD27−), and related cytokines in LN patients with multiple relapses (MR) (n = 15) and no relapse (NR) (n = 15) during disease remission. The expression of inhibitory/adhesion molecules, cell proliferation and calcium mobilization in classical memory and exhausted B cells were also assessed. The MR group had higher proportion of circulating exhausted and classical memory B cells compared to the NR group and healthy controls (HC) (p all <0.05 for MR vs. NR or HC). Blood levels of IL-6, BAFF, IL-21, CD62L, CXCR3 and Siglec-6 were all higher in the MR group (p < 0.05, for all). Exhausted B cells from the MR group showed higher FcRL4, CD22, CD85j and CD183 but lower CD62L expression than NR and HC groups. Exhausted B cells from MR patients exhibited reduced proliferation compared to NR patients and HC, while classical memory B cell proliferation in MR group was higher than the other two groups. Exhausted B cells from both MR and NR patients showed impaired calcium mobilization. Alterations in exhausted and classical memory B cells are related to disease relapse in LN. These findings may help devise new strategies for monitoring disease activity and preventing relapse in LN.

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