采用单倍体相合自然杀伤细胞和抗GD2单克隆抗体m3F8进行过继性免疫治疗难治性神经母细胞瘤:一项I期研究的结果
Adoptive immunotherapy with haploidentical natural killer cells and Anti-GD2 monoclonal antibody m3F8 for resistant neuroblastoma: Results of a phase I study.
作者信息
Modak Shakeel, Le Luduec Jean-Benoit, Cheung Irene Y, Goldman Debra A, Ostrovnaya Irina, Doubrovina Ekaterina, Basu Ellen, Kushner Brian H, Kramer Kim, Roberts Stephen S, O'Reilly Richard J, Cheung Nai-Kong V, Hsu Katharine C
机构信息
Department of Pediatrics, Memorial Sloan Kettering Cancer Center, New York, NY.
Immunology Program, Sloan-Kettering Institute for Cancer Research, New York, NY.
出版信息
Oncoimmunology. 2018 May 10;7(8):e1461305. doi: 10.1080/2162402X.2018.1461305. eCollection 2018.
Natural killer (NK) cell-mediated antibody-dependent toxicity is a potent mechanism of action of the anti-GD2 murine monoclonal antibody 3F8 (m3F8). Killer immunoglobulin-like receptor (KIR) and HLA genotypes modulate NK activity and are key prognostic markers in m3F8-treated patients with neuroblastoma. Endogenous NK-cells are suppressed in the setting of high tumor burden and chemotherapy. Allogeneic NK-cells however, demonstrate potent anti-neuroblastoma activity. We report on the results of a phase I clinical trial of haploidentical NK-cells plus m3F8 administered to patients with high-risk neuroblastoma after conditioning chemotherapy. The primary objective was to determine the maximum tolerated NK-cell dose (MTD). Secondary objectives included assessing anti-neuroblastoma activity and its relationship to donor-recipient KIR/HLA genotypes, NK function, and donor NK chimerism. Patients received a lymphodepleting regimen prior to infusion of haploidentical CD3-CD56+ NK-cells, followed by m3F8. Overall and progression free survival (PFS) were assessed from the time of first NK-cell dose. Univariate Cox regression assessed relationship between dose and outcomes. Thirty-five patients received NK-cells at one of five dose levels ranging from <1×10 to 50×10 CD3-CD56+cells/kg. One patient experienced grade 3 hypertension and grade 4 pneumonitis. MTD was not reached. Ten patients (29%) had complete or partial response; 17 (47%) had no response; and eight (23%) had progressive disease. No relationship was found between response and KIR/HLA genotype or between response and FcγRIII receptor polymorphisms. Patients receiving >10×10 CD56+cells/kg had improved PFS (HR: 0.36, 95%CI: 0.15-0.87, p = 0.022). Patient NK-cells displayed high NKG2A expression, leading to inhibition by HLA-E-expressing neuroblastoma cells. Adoptive NK-cell therapy in combination with m3F8 is safe and has anti-neuroblastoma activity at higher cell doses.
自然杀伤(NK)细胞介导的抗体依赖性毒性是抗GD2鼠单克隆抗体3F8(m3F8)的一种有效作用机制。杀伤免疫球蛋白样受体(KIR)和HLA基因型调节NK活性,并且是接受m3F8治疗的神经母细胞瘤患者的关键预后标志物。在高肿瘤负荷和化疗情况下,内源性NK细胞受到抑制。然而,同种异体NK细胞表现出强大的抗神经母细胞瘤活性。我们报告了一项I期临床试验的结果,该试验对接受预处理化疗后的高危神经母细胞瘤患者给予单倍体NK细胞加m3F8。主要目的是确定最大耐受NK细胞剂量(MTD)。次要目的包括评估抗神经母细胞瘤活性及其与供体-受体KIR/HLA基因型、NK功能和供体NK嵌合体的关系。患者在输注单倍体CD3-CD56+NK细胞之前接受淋巴细胞清除方案,随后给予m3F8。从首次给予NK细胞剂量时开始评估总生存期和无进展生存期(PFS)。单变量Cox回归评估剂量与结局之间的关系。35例患者接受了5个剂量水平之一的NK细胞,剂量范围从<1×10到50×10 CD3-CD56+细胞/kg。1例患者出现3级高血压和4级肺炎。未达到MTD。10例患者(29%)有完全或部分缓解;17例(47%)无反应;8例(23%)疾病进展。未发现反应与KIR/HLA基因型之间或反应与FcγRIII受体多态性之间存在关联。接受>10×10 CD56+细胞/kg的患者PFS有所改善(HR:0.36,95%CI:0.15-0.87,p = 0.022)。患者NK细胞显示高NKG2A表达,导致被表达HLA-E的神经母细胞瘤细胞抑制。过继性NK细胞疗法联合m3F8是安全的,并且在较高细胞剂量下具有抗神经母细胞瘤活性。
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