Department of Immunobiology, Biomedical Primate Research Centre, 2280 GH Rijswijk, The Netherlands;
J Immunol. 2014 May 1;192(9):4242-53. doi: 10.4049/jimmunol.1303125. Epub 2014 Apr 2.
Depleting mAbs against the pan B cell marker CD20 are remarkably effective in the treatment of autoimmune-mediated inflammatory disorders, but the underlying mechanisms are poorly defined. The primary objective of this study was to find a mechanistic explanation for the remarkable clinical effect of the anti-CD20 mAbs in a representative nonhuman primate autoimmune-mediated inflammatory disorder model, experimental autoimmune encephalomyelitis (EAE) in common marmosets, allowing detailed analysis of secondary lymphoid organs (SLO). We observed that the depletion of CD20(+) B cells creates a less immunostimulatory environment in the SLO reflected by reduced expression of MHC class II, CD40, CD83, and CD80/CD86. APCs isolated from SLO of B cell-depleted EAE monkeys were also less responsive to mitogenic stimulation. The depleted B cell areas were replenished by T cells, of which the majority expressed CD127 (IL-7R) and CCR7. Such effects were not detected in EAE marmosets treated with mAb against BLyS or APRIL, where B cell depletion via withdrawal of essential survival cytokines was not associated with a marked clinical effect. We propose that at least part of the efficacy of anti-CD20 mAb therapy is attributable to the sustained CCR7 expression on T cells within SLO, limiting their release into the circulation.
耗竭 pan B 细胞标记物 CD20 的单抗在治疗自身免疫介导的炎症性疾病方面非常有效,但潜在机制仍不清楚。本研究的主要目的是为抗 CD20 单抗在有代表性的非人灵长类动物自身免疫介导的炎症性疾病模型,即食蟹猴实验性自身免疫性脑脊髓炎 (EAE) 中的显著临床疗效找到一种机制解释,从而能够对次级淋巴器官 (SLO) 进行详细分析。我们观察到,CD20(+)B 细胞耗竭会导致 SLO 中的免疫刺激环境减弱,表现为 MHC Ⅱ类、CD40、CD83 和 CD80/CD86 的表达减少。从 B 细胞耗竭性 EAE 猴 SLO 中分离出的 APC 对有丝分裂刺激的反应性也降低。耗竭的 B 细胞区域被 T 细胞补充,其中大多数表达 CD127(IL-7R)和 CCR7。在接受 BLyS 或 APRIL 单抗治疗的 EAE 食蟹猴中未检测到这种效应,因为通过去除必需的生存细胞因子来耗竭 B 细胞与显著的临床疗效无关。我们提出,抗 CD20 单抗治疗的至少部分疗效归因于 SLO 内 T 细胞上持续的 CCR7 表达,限制了它们释放到循环中。
