High Expression of the Costimulatory Checkpoint Factor DNAM-1 by CD4+ T-Cells from Multiple Myeloma Patients Refractory to Daratumumab-Containing Regimens.

Clinical Hematology International Pub Date : 2022-09-01 Epub Date: 2022-08-09 DOI:10.1007/s44228-022-00013-7
Katrine Fladeland Iversen, Line Nederby, Thomas Lund, Torben Plesner
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Abstract

Multiple myeloma is an incurable disease characterized by unregulated growth of malignant plasma cells in the bone marrow (BM). Tumor-induced dysfunction of T-cells may be responsible for immune evasion and failure of immunotherapy. Therefore, a better understanding of the phenotype of T-cells at the tumor site is needed. We assessed the expression of immune regulatory receptors on T-cell subsets from peripheral blood (PB) and BM using multicolor flow cytometry. Paired PB and BM samples were collected from newly diagnosed, treatment-naïve myeloma patients (n = 19) and patients progressing during treatment with the CD38 monoclonal antibody daratumumab alone or in combination with other anti-myeloma drugs (n = 39). We observed that CD4+ T-cells from both PB and BM of patients relapsing on daratumumab have a higher expression of the costimulatory checkpoint receptor DNAM-1. The potential role of DNAM-1+CD4+ T-cells in the development of resistance to daratumumab needs further exploration. We also observed that the inhibitory checkpoint receptor TIGIT is more frequently expressed by BM CD8+ T-cells from myeloma patients than PD-1 and CTLA-4, which supports the hypothesis that TIGIT may play a central role in the immune escape of the malignant plasma cells.

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对含daratumumab治疗方案难治性多发性骨髓瘤患者CD4+ t细胞中共刺激检查点因子DNAM-1的高表达
多发性骨髓瘤是一种无法治愈的疾病,其特征是骨髓中恶性浆细胞(BM)生长不受调节。肿瘤诱导的t细胞功能障碍可能是免疫逃避和免疫治疗失败的原因。因此,需要更好地了解肿瘤部位t细胞的表型。我们使用多色流式细胞术评估了外周血(PB)和BM中免疫调节受体在t细胞亚群上的表达。从新诊断的treatment-naïve骨髓瘤患者(n = 19)和在单独使用CD38单克隆抗体daratumumab或联合其他抗骨髓瘤药物治疗期间进展的患者(n = 39)中收集成对的PB和BM样本。我们观察到,服用达拉单抗复发的PB和BM患者的CD4+ t细胞表达更高的共刺激检查点受体DNAM-1。DNAM-1+CD4+ t细胞在daratumumab耐药发展中的潜在作用有待进一步探索。我们还观察到,来自骨髓瘤患者的BM CD8+ t细胞比PD-1和CTLA-4更频繁地表达抑制检查点受体TIGIT,这支持了TIGIT可能在恶性浆细胞的免疫逃逸中发挥核心作用的假设。
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