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贝利尤单抗促进系统性红斑狼疮患者中激活的自身反应性 B 细胞的阴性选择。

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

机构信息

Center for Autoimmunity and Musculoskeletal and Hematologic Diseases, and.

Biostatistics Unit, Feinstein Institute for Medical Research, Manhasset, New York, New York, USA.

出版信息

JCI Insight. 2018 Sep 6;3(17). doi: 10.1172/jci.insight.122525.

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.

摘要

贝利尤单抗对活跃的系统性红斑狼疮(SLE)具有治疗益处,尤其对高滴度抗 dsDNA 抗体的患者。我们想知道贝利尤单抗治疗的 SLE 患者中 B 细胞大量丢失是否伴随着免疫球蛋白库的变化。我们招募了 15 名持续接受贝利尤单抗治疗超过 7 年的患者、17 名匹配的对照者和 5 名在药物开始使用前后进行研究的患者。对分选纯化的成熟 B 细胞和浆母细胞的 VH 基因进行了下一代测序。我们发现 B 细胞激活因子(BAFF)调节过渡性 B 细胞检查点,在慢性贝利尤单抗治疗后,过渡性 1(T1)细胞得到保留,T3 和幼稚 B 细胞丢失约 90%。类别转换的记忆 B 细胞、B1 B 细胞和浆母细胞也大量耗竭。下一代测序未显示 VH、DH 或 JH 家族使用的重新分布,也未显示贝利尤单抗对未突变 IgM 序列中自身反应性 VH4-34 基因或 CDR3 组成的代表性产生影响,这表明对幼稚 B 细胞库的选择影响很小。有趣的是,在慢性贝利尤单抗治疗的患者中,突变 IgM 和浆母细胞序列中的 VH4-34 丢失明显大于对照者,这表明贝利尤单抗促进了激活的自身反应性 B 细胞的阴性选择。

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