一种新型抗 CD19 单克隆抗体(GBR 401),对 B 细胞恶性肿瘤具有高杀伤活性。
A novel anti-CD19 monoclonal antibody (GBR 401) with high killing activity against B cell malignancies.
机构信息
Service and Central Laboratory of Hematology, University Hospital of Lausanne, Rue du Bugnon 46, 1011- CHUV, Lausanne, Switzerland.
出版信息
J Hematol Oncol. 2014 Apr 14;7:33. doi: 10.1186/1756-8722-7-33.
BACKGROUND
CD19 is a B cell lineage specific surface receptor whose broad expression, from pro-B cells to early plasma cells, makes it an attractive target for the immunotherapy of B cell malignancies. In this study we present the generation of a novel humanized anti-CD19 monoclonal antibody (mAb), GBR 401, and investigate its therapeutic potential on human B cell malignancies.
METHODS
GBR 401 was partially defucosylated in order to enhance its cytotoxic function. We analyzed the in vitro depleting effects of GBR 401 against B cell lines and primary malignant B cells from patients in the presence or in absence of purified NK cells isolated from healthy donors. In vivo, the antibody dependent cellular cytotoxicity (ADCC) efficacy of GBR 401 was assessed in a B cell depletion model consisting of SCID mice injected with healthy human donor PBMC, and a malignant B cell depletion model where SCID mice are xenografted with both primary human B-CLL tumors and heterologous human NK cells. Furthermore, the anti-tumor activity of GBR 401 was also evaluated in a xenochimeric mouse model of human Burkitt lymphoma using mice xenografted intravenously with Raji cells. Pharmacological inhibition tests were used to characterize the mechanism of the cell death induced by GBR 401.
RESULTS
GBR 401 exerts a potent in vitro and in vivo cytotoxic activity against primary samples from patients representing various B-cell malignancies. GBR 401 elicits a markedly higher level of ADCC on primary malignant B cells when compared to fucosylated similar mAb and to Rituximab, the current anti-CD20 mAb standard immunotherapeutic treatment for B cell malignancies, showing killing at 500 times lower concentrations. Of interest, GBR 401 also exhibits a potent direct killing effect in different malignant B cell lines that involves homotypic aggregation mediated by actin relocalization.
CONCLUSION
These results contribute to consolidate clinical interest in developing GBR 401 for treatment of hematopoietic B cell malignancies, particularly for patients refractory to anti-CD20 mAb therapies.
背景
CD19 是 B 细胞谱系特异性表面受体,其广泛表达于前 B 细胞至早期浆细胞,使其成为 B 细胞恶性肿瘤免疫治疗的一个有吸引力的靶点。在这项研究中,我们介绍了一种新型人源化抗 CD19 单克隆抗体(mAb)GBR 401 的产生,并研究了其对人类 B 细胞恶性肿瘤的治疗潜力。
方法
为了增强其细胞毒性作用,GBR 401 被部分去岩藻糖基化。我们分析了 GBR 401 在存在或不存在从健康供体中分离的纯化 NK 细胞的情况下,对 B 细胞系和来自患者的原代恶性 B 细胞的体外清除作用。在体内,我们在由注射健康人供体 PBMC 的 SCID 小鼠组成的 B 细胞耗竭模型中评估了 GBR 401 的抗体依赖性细胞毒性(ADCC)功效,以及在 SCID 小鼠异种移植原发性人 B-CLL 肿瘤和异源人 NK 细胞的恶性 B 细胞耗竭模型中评估了 GBR 401 的抗瘤活性。此外,我们还在使用静脉注射 Raji 细胞异种移植的异种嵌合小鼠模型中评估了 GBR 401 对人 Burkitt 淋巴瘤的抗肿瘤活性。我们使用药理学抑制试验来表征 GBR 401 诱导细胞死亡的机制。
结果
GBR 401 对来自代表各种 B 细胞恶性肿瘤的患者的原代样本表现出强大的体外和体内细胞毒性活性。与岩藻糖基化的类似 mAb 和目前用于 B 细胞恶性肿瘤的抗 CD20 mAb 标准免疫治疗药物利妥昔单抗相比,GBR 401 对原代恶性 B 细胞诱导的 ADCC 水平明显更高,其杀伤浓度低 500 倍。有趣的是,GBR 401 还在不同的恶性 B 细胞系中表现出强大的直接杀伤作用,涉及由肌动蛋白重定位介导的同质聚集。
结论
这些结果有助于巩固开发 GBR 401 用于治疗造血 B 细胞恶性肿瘤的临床兴趣,特别是对于对抗 CD20 mAb 治疗有抗性的患者。
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