在自身免疫中靶向BMI-1消耗抗体分泌细胞

IF 4.6 2区 医学 Q2 IMMUNOLOGY
Jack Polmear, Lauren Hailes, Moshe Olshansky, Maureen Rischmueller, Elan L'Estrange-Stranieri, Anne L Fletcher, Margaret L Hibbs, Vanessa L Bryant, Kim L Good-Jacobson
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引用次数: 0

摘要

在系统性红斑狼疮(SLE)和Sjögren综合征等自身免疫性疾病中,B细胞驱动自身反应性抗体分泌细胞(ASCs)的产生,导致长期器官损伤。目前针对抗体介导的自身免疫性疾病的治疗是靶向B细胞或广泛抑制免疫系统。然而,先前存在的长寿命ASCs通常难以治疗,留下了一个自身反应性细胞库,继续产生抗体。因此,开发针对ASCs的新型治疗方法对于改善患者预后至关重要。我们的目的是测试靶向表观遗传调节剂BMI-1是否可以在体内和体外的自身免疫性疾病中消耗ASCs。方法研究BMI-1抑制剂在小鼠和人自身免疫性疾病中的应用。在评估ASCs、血清抗体和免疫复合物之前,用BMI-1小分子抑制剂PTC-028治疗SLE模型Lyn - / -小鼠。为了检测人类ASC的存活,建立了一种新的基于人成纤维细胞的检测方法,并评估了PTC-028对Sjögren综合征患者ASC的影响。结果抑制BMI-1可显著降低Lyn - / -小鼠脾和骨髓ASCs。ASCs的下降与细胞周期基因表达异常有关,并导致血清IgG3、免疫复合物和抗dna IgG的显著下降。PTC-028在降低Sjögren综合征患者和年龄匹配的健康供体的离体浆细胞存活率方面也有效。结论这些数据表明,抑制BMI-1可在多种情况下消耗ASC,因此BMI-1是抗体介导的自身免疫性疾病的可行治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Targeting BMI-1 to deplete antibody-secreting cells in autoimmunity

Targeting BMI-1 to deplete antibody-secreting cells in autoimmunity

Objectives

B cells drive the production of autoreactive antibody-secreting cells (ASCs) in autoimmune diseases such as Systemic Lupus Erythematosus (SLE) and Sjögren's syndrome, causing long-term organ damage. Current treatments for antibody-mediated autoimmune diseases target B cells or broadly suppress the immune system. However, pre-existing long-lived ASCs are often refractory to treatment, leaving a reservoir of autoreactive cells that continue to produce antibodies. Therefore, the development of novel treatment methods targeting ASCs is vital to improve patient outcomes. Our objective was to test whether targeting the epigenetic regulator BMI-1 could deplete ASCs in autoimmune conditions in vivo and in vitro.

Methods

Use of a BMI-1 inhibitor in both mouse and human autoimmune settings was investigated. Lyn−/− mice, a model of SLE, were treated with the BMI-1 small molecule inhibitor PTC-028, before assessment of ASCs, serum antibody and immune complexes. To examine human ASC survival, a novel human fibroblast-based assay was established, and the impact of PTC-028 on ASCs derived from Sjögren's syndrome patients was evaluated.

Results

BMI-1 inhibition significantly decreased splenic and bone marrow ASCs in Lyn−/− mice. The decline in ASCs was linked to aberrant cell cycle gene expression and led to a significant decrease in serum IgG3, immune complexes and anti-DNA IgG. PTC-028 was also efficacious in reducing ex vivo plasma cell survival from both Sjögren's syndrome patients and age-matched healthy donors.

Conclusion

These data provide evidence that inhibiting BMI-1 can deplete ASC in a variety of contexts and thus BMI-1 is a viable therapeutic target for antibody-mediated autoimmune diseases.

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来源期刊
Clinical & Translational Immunology
Clinical & Translational Immunology Medicine-Immunology and Allergy
CiteScore
12.00
自引率
1.70%
发文量
77
审稿时长
13 weeks
期刊介绍: Clinical & Translational Immunology is an open access, fully peer-reviewed journal devoted to publishing cutting-edge advances in biomedical research for scientists and physicians. The Journal covers fields including cancer biology, cardiovascular research, gene therapy, immunology, vaccine development and disease pathogenesis and therapy at the earliest phases of investigation.
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