综合分析揭示 CD38 是富含浆细胞的前期疾病和已确诊的类风湿关节炎及系统性红斑狼疮的治疗靶点。

Integrative analysis reveals CD38 as a therapeutic target for plasma cell-rich pre-disease and established rheumatoid arthritis and systemic lupus erythematosus.

机构信息

Immunology, Janssen Research, 1400 McKean Road, Spring House, PA, 19477, USA.

Rheumatology Unit, Repatriation General Hospital and Flinders University, Adelaide, Australia.

出版信息

Arthritis Res Ther. 2018 May 2;20(1):85. doi: 10.1186/s13075-018-1578-z.

DOI:10.1186/s13075-018-1578-z

PMID:29720240

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5932888/

Abstract

BACKGROUND

Plasmablasts and plasma cells play a key role in many autoimmune diseases, such as rheumatoid arthritis (RA) and systemic lupus erythematosus (SLE). This study was undertaken to evaluate the potential of targeting CD38 as a plasma cell/plasmablast depletion mechanism by daratumumab in the treatment of patients with RA and SLE.

METHODS

RNA-sequencing analysis of synovial biopsies from various stages of RA disease progression, flow cytometry analysis of peripheral blood mononuclear cells (PBMC) from patients with RA or SLE and healthy donors, immunohistochemistry assessment (IHC) of synovial biopsies from patients with early RA, and ex vivo immune cell depletion assays using daratumumab (an anti-CD38 monoclonal antibody) were used to assess CD38 as a therapeutic target.

RESULTS

We demonstrated that the plasma cell/plasmablast-related genes CD38, XBP1, IRF4, PRDM1, IGJ and TNFSF13B are significantly up-regulated in synovial biopsies from patients with arthralgia, undifferentiated arthritis (UA), early RA and established RA as compared to healthy controls and control patients with osteoarthritis. In addition, the highest CD38 expression was observed on plasma cells and plasmablasts compared to natural killer (NK) cells, classical dendritic cells (DCs), plasmacytoid DCs (pDCs) and T cells, in blood from healthy controls and patients with SLE and RA. Furthermore, IHC showed CD38 staining in the same region as CD3 and CD138 staining in synovial tissue biopsies from patients with early RA. Most importantly, our data show for the first time that daratumumab effectively depletes plasma cells/plasmablasts in PBMC from patients with SLE and RA in a dose-dependent manner ex vivo.

CONCLUSION

These results indicate that CD38 may be a potential target for RA disease interception and daratumumab should be evaluated clinically for the treatment of both RA and SLE.

摘要

背景

浆细胞和浆母细胞在许多自身免疫性疾病中发挥着关键作用，如类风湿关节炎（RA）和系统性红斑狼疮（SLE）。本研究旨在评估达雷妥尤单抗通过靶向 CD38 作为一种浆细胞/浆母细胞耗竭机制在 RA 和 SLE 患者治疗中的潜力。

方法

对 RA 疾病进展的各个阶段的滑膜活检进行 RNA 测序分析，对 RA 或 SLE 患者和健康供体的外周血单个核细胞（PBMC）进行流式细胞术分析，对早期 RA 患者的滑膜活检进行免疫组织化学评估（IHC），并使用达雷妥尤单抗（一种抗 CD38 单克隆抗体）进行体外免疫细胞耗竭测定，以评估 CD38 作为治疗靶点。

结果

我们证明了与健康对照和对照骨关节炎患者相比，在患有关节痛、未分化关节炎（UA）、早期 RA 和确诊 RA 的患者的滑膜活检中，浆细胞/浆母细胞相关基因 CD38、XBP1、IRF4、PRDM1、IGJ 和 TNFSF13B 显著上调。此外，与健康对照者和 RA 和 SLE 患者的血液中的自然杀伤（NK）细胞、经典树突状细胞（DC）、浆细胞样 DC（pDC）和 T 细胞相比，CD38 在血浆细胞和浆母细胞上的表达最高。此外，IHC 显示在早期 RA 患者的滑膜组织活检中，CD38 染色与 CD3 和 CD138 染色位于同一区域。最重要的是，我们的数据首次表明，达雷妥尤单抗可在体外以剂量依赖性方式有效耗竭 SLE 和 RA 患者 PBMC 中的浆细胞/浆母细胞。

结论

这些结果表明，CD38 可能是 RA 疾病干预的潜在靶点，应在临床上评估达雷妥尤单抗治疗 RA 和 SLE 的效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d2ce/5932888/2b4067bb170f/13075_2018_1578_Fig1_HTML.jpg

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综合分析揭示 CD38 是富含浆细胞的前期疾病和已确诊的类风湿关节炎及系统性红斑狼疮的治疗靶点。

Integrative analysis reveals CD38 as a therapeutic target for plasma cell-rich pre-disease and established rheumatoid arthritis and systemic lupus erythematosus.

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