达雷妥尤单抗可清除CD38+免疫调节细胞,促进T细胞扩增,并使多发性骨髓瘤中的T细胞库发生偏移。
Daratumumab depletes CD38+ immune regulatory cells, promotes T-cell expansion, and skews T-cell repertoire in multiple myeloma.
作者信息
Krejcik Jakub, Casneuf Tineke, Nijhof Inger S, Verbist Bie, Bald Jaime, Plesner Torben, Syed Khaja, Liu Kevin, van de Donk Niels W C J, Weiss Brendan M, Ahmadi Tahamtan, Lokhorst Henk M, Mutis Tuna, Sasser A Kate
机构信息
Department of Hematology, VU University Medical Center, Amsterdam, The Netherlands; Institute of Regional Health Science and Department of Hematology, Sections of Internal Medicine, Vejle Hospital and University of Southern Denmark, Vejle, Denmark;
Janssen Research & Development, Beerse, Belgium;
出版信息
Blood. 2016 Jul 21;128(3):384-94. doi: 10.1182/blood-2015-12-687749. Epub 2016 May 24.
Daratumumab targets CD38-expressing myeloma cells through a variety of immune-mediated mechanisms (complement-dependent cytotoxicity, antibody-dependent cell-mediated cytotoxicity, and antibody-dependent cellular phagocytosis) and direct apoptosis with crosslinking. These mechanisms may also target nonplasma cells that express CD38, which prompted evaluation of daratumumab's effects on CD38-positive immune subpopulations. Peripheral blood (PB) and bone marrow (BM) from patients with relapsed/refractory myeloma from 2 daratumumab monotherapy studies were analyzed before and during therapy and at relapse. Regulatory B cells and myeloid-derived suppressor cells, previously shown to express CD38, were evaluated for immunosuppressive activity and daratumumab sensitivity in the myeloma setting. A novel subpopulation of regulatory T cells (Tregs) expressing CD38 was identified. These Tregs were more immunosuppressive in vitro than CD38-negative Tregs and were reduced in daratumumab-treated patients. In parallel, daratumumab induced robust increases in helper and cytotoxic T-cell absolute counts. In PB and BM, daratumumab induced significant increases in CD8(+):CD4(+) and CD8(+):Treg ratios, and increased memory T cells while decreasing naïve T cells. The majority of patients demonstrated these broad T-cell changes, although patients with a partial response or better showed greater maximum effector and helper T-cell increases, elevated antiviral and alloreactive functional responses, and significantly greater increases in T-cell clonality as measured by T-cell receptor (TCR) sequencing. Increased TCR clonality positively correlated with increased CD8(+) PB T-cell counts. Depletion of CD38(+) immunosuppressive cells, which is associated with an increase in T-helper cells, cytotoxic T cells, T-cell functional response, and TCR clonality, represents possible additional mechanisms of action for daratumumab and deserves further exploration.
达雷妥尤单抗通过多种免疫介导机制(补体依赖的细胞毒性、抗体依赖的细胞介导的细胞毒性和抗体依赖的细胞吞噬作用)靶向表达CD38的骨髓瘤细胞,并通过交联直接诱导细胞凋亡。这些机制也可能靶向表达CD38的非浆细胞,这促使人们评估达雷妥尤单抗对CD38阳性免疫亚群的影响。对两项达雷妥尤单抗单药治疗研究中复发/难治性骨髓瘤患者的外周血(PB)和骨髓(BM)在治疗前、治疗期间及复发时进行了分析。对之前已证明表达CD38的调节性B细胞和髓源性抑制细胞在骨髓瘤环境中的免疫抑制活性和对达雷妥尤单抗的敏感性进行了评估。鉴定出了一个表达CD38的新型调节性T细胞(Tregs)亚群。这些Tregs在体外比CD38阴性的Tregs具有更强的免疫抑制作用,并且在接受达雷妥尤单抗治疗的患者中数量减少。同时,达雷妥尤单抗使辅助性和细胞毒性T细胞的绝对计数显著增加。在PB和BM中,达雷妥尤单抗使CD8(+)∶CD4(+)和CD8(+)∶Treg比值显著增加,使记忆性T细胞增加,而使初始T细胞减少。大多数患者表现出这些广泛的T细胞变化,尽管部分缓解或更好疗效的患者显示出最大效应性和辅助性T细胞增加幅度更大、抗病毒和同种异体反应性功能反应增强,并且通过T细胞受体(TCR)测序测量的T细胞克隆性显著增加。TCR克隆性增加与CD8(+) PB T细胞计数增加呈正相关。CD38(+)免疫抑制细胞的耗竭与辅助性T细胞、细胞毒性T细胞、T细胞功能反应和TCR克隆性增加相关,这代表了达雷妥尤单抗可能的额外作用机制,值得进一步探索。
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