Literature DB >> 30185675

Belimumab promotes negative selection of activated autoreactive B cells in systemic lupus erythematosus patients.

Weiqing Huang1, Tam D Quach1, Cosmin Dascalu1, Zheng Liu1, Tungming Leung2, Miranda Byrne-Steele3, Wenjing Pan3, Qunying Yang3, Jian Han3, Martin Lesser2, Thomas L Rothstein4, Richard Furie5, Meggan Mackay1,5, Cynthia Aranow1,5, Anne Davidson1,5.   

Abstract

Belimumab has therapeutic benefit in active systemic lupus erythematosus (SLE), especially in patients with high-titer anti-dsDNA antibodies. We asked whether the profound B cell loss in belimumab-treated SLE patients is accompanied by shifts in the immunoglobulin repertoire. We enrolled 15 patients who had been continuously treated with belimumab for more than 7 years, 17 matched controls, and 5 patients who were studied before and after drug initiation. VH genes of sort-purified mature B cells and plasmablasts were subjected to next-generation sequencing. We found that B cell-activating factor (BAFF) regulates the transitional B cell checkpoint, with conservation of transitional 1 (T1) cells and approximately 90% loss of T3 and naive B cells after chronic belimumab treatment. Class-switched memory B cells, B1 B cells, and plasmablasts were also substantially depleted. Next-generation sequencing revealed no redistribution of VH, DH, or JH family usage and no effect of belimumab on representation of the autoreactive VH4-34 gene or CDR3 composition in unmutated IgM sequences, suggesting a minimal effect on selection of the naive B cell repertoire. Interestingly, a significantly greater loss of VH4-34 was observed among mutated IgM and plasmablast sequences in chronic belimumab-treated subjects than in controls, suggesting that belimumab promotes negative selection of activated autoreactive B cells.

Entities:  

Keywords:  Autoimmunity; B cells; Immunology; Tolerance

Mesh:

Substances:

Year:  2018        PMID: 30185675      PMCID: PMC6171800          DOI: 10.1172/jci.insight.122525

Source DB:  PubMed          Journal:  JCI Insight        ISSN: 2379-3708


  59 in total

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