CD16NK-92 和抗 CD123 单克隆抗体延长原发性人急性髓系白血病异种移植小鼠的生存期。

CD16NK-92 and anti-CD123 monoclonal antibody prolongs survival in primary human acute myeloid leukemia xenografted mice.

机构信息

Cell Therapy Program, Princess Margaret Cancer Centre, Toronto, Ontario, Canada

Institute of Medical Science, University of Toronto, Ontario, Canada.

出版信息

Haematologica. 2018 Oct;103(10):1720-1729. doi: 10.3324/haematol.2017.187385. Epub 2018 Jul 5.

Patients with acute myeloid leukemia (AML) often relapse after initial therapy because of persistence of leukemic stem cells that frequently express the IL-3 receptor alpha chain CD123. Natural killer (NK) cell-based therapeutic strategies for AML show promise and we explore the NK cell lines, NK-92 and CD16 NK-92, as a treatment for AML. NK-92 has been tested in phase I clinical trials with minimal toxicity; irradiation prior to infusion prevents risk of engraftment. The CD16 negative NK-92 parental line was genetically modified to express the high affinity Fc gamma receptor, enabling antibody-dependent cell-mediated cytotoxicity, which we utilized in combination with an anti-CD123 antibody to target leukemic stem cells. NK-92 was preferentially cytotoxic against leukemic stem and progenitor cells compared with bulk leukemia in in vitro assays, while CD16 NK-92 in combination with an anti-CD123 mAb mediated antibody-dependent cell-mediated cytotoxicity against CD123 leukemic targets. Furthermore, NK-92 infusions (with or without prior irradiation) improved survival in a primary AML xenograft model. Mice xenografted with primary human AML cells had a superior survival when treated with irradiated CD16NK-92 cells and an anti-CD123 monoclonal antibody (7G3) versus treatment with irradiated CD16NK-92 cells combined with an isotype control antibody. In this proof-of-principle study, we show for the first time that a CD16NK-92 cell line combined with an antibody that targets a leukemic stem cell antigen can lead to improved survival in a relevant pre-clinical model of AML.

急性髓细胞白血病 (AML) 患者在初始治疗后常因白血病干细胞的持续存在而复发，这些干细胞通常表达白细胞介素 3 受体 alpha 链 CD123。基于自然杀伤 (NK) 细胞的 AML 治疗策略显示出前景，我们探索了 NK 细胞系 NK-92 和 CD16 NK-92，作为 AML 的治疗方法。NK-92 已在 I 期临床试验中进行了测试，毒性极小；输注前照射可防止移植物植入的风险。CD16 阴性 NK-92 亲本系经过基因修饰表达高亲和力 Fcγ受体，从而能够进行抗体依赖性细胞介导的细胞毒性，我们将其与抗 CD123 抗体结合用于靶向白血病干细胞。在体外实验中，NK-92 对白血病干细胞和祖细胞的细胞毒性优于 bulk 白血病，而 CD16 NK-92 与抗 CD123 mAb 结合可介导针对 CD123 白血病靶标的抗体依赖性细胞介导的细胞毒性。此外，NK-92 输注（无论是否事先照射）可改善原发性 AML 异种移植模型中的存活率。用照射后的 CD16NK-92 细胞和抗 CD123 单克隆抗体（7G3）治疗与用照射后的 CD16NK-92 细胞联合同种型对照抗体治疗的原发性人 AML 细胞异种移植小鼠的存活率更高。在这项初步研究中，我们首次表明，CD16NK-92 细胞系与靶向白血病干细胞抗原的抗体结合可导致相关 AML 临床前模型中的存活率提高。