在现行良好生产规范条件下，对高细胞毒性的人自然杀伤细胞92细胞系进行体外扩增，用于临床过继性细胞免疫治疗。

Ex vivo expansion of the highly cytotoxic human natural killer-92 cell-line under current good manufacturing practice conditions for clinical adoptive cellular immunotherapy.

作者信息

Tam Y K, Martinson J A, Doligosa K, Klingemann H-G

机构信息

Section of Bone Marrow Transplant and Cell Therapy, Rush Presbyterian-St Luke's Medical Center, Rush Medical School, Chicago, IL 60612, USA.

出版信息

Cytotherapy. 2003;5(3):259-72. doi: 10.1080/14653240310001523.

DOI:10.1080/14653240310001523

PMID:12850795

Abstract

BACKGROUND

Adoptive transfer of ex vivo expanded cytotoxic immune cells has become a viable strategy for treatment of malignant disease. Natural killer (NK)-92, a highly cytotoxic, IL2-dependent human NK cell-line, is an excellent candidate as an immunotherapeutic agent, being active for prolonged periods following irradiation and IL2 deprivation, non-toxic and non-immunogenic, and easily expanded. A number of clinical trials using NK-92 for different indications are currently underway. The aim of this study was to develop current good manufacturing practice (cGMP)-compliant expansion methodology for NK-92.

METHODS

The ability to expand NK-92 ex vivo was evaluated. Serum-free culture media, as well as media supplements (IL2, serum/plasma/albumin), culture containers and feeding regimens were compared for their ability to support expansion, viability and cytotoxicity of NK-92 cells.

RESULTS

NK-92 cells can be expanded in X-Vivo 10 serum-free media with 500 U/mL of rhIL2 (Proleukin), and 2.5% human serum/plasma to achieve concentrations sufficient to treat patients with >5210(10) cells. The protocol involves cultures initiated at 2.5210(5) cells/mL in 25 mL in 1 L Vuelife culture bags, with addition of fresh media plus IL2 every 3 days to maintain an optimal density of NK-92 cells for expansion. Daily disruption of cell aggregates enhances NK-92 cells expansion and viability during the culture period. Final yields of approximately 1.1-1.3210(6) cells/mL in a 1.2 L volume (1.36-1.56210(9) cells; 218-250 fold expansion) over 15-17 days is achievable under cGMP-compliant conditions with >85% viability. The feasibility of this approach has been shown in ongoing clinical trial with NK-92.

DISCUSSION

We describe a protocol that allows for >200-fold expansion of NK-92 cells within a 2-2.5 week period under GMP standards, in quality and quantity suitable for clinical adoptive immunotherapy.

摘要

背景

体外扩增的细胞毒性免疫细胞的过继性转移已成为治疗恶性疾病的一种可行策略。自然杀伤（NK）-92是一种高度细胞毒性、依赖白细胞介素2（IL2）的人NK细胞系，作为一种免疫治疗剂是极佳的候选者，在照射和剥夺IL2后仍能长时间保持活性，无毒且无免疫原性，并且易于扩增。目前正在进行多项使用NK-92治疗不同适应症的临床试验。本研究的目的是开发符合现行药品生产质量管理规范（cGMP）的NK-92扩增方法。

方法

评估NK-92体外扩增的能力。比较无血清培养基以及培养基补充剂（IL2、血清/血浆/白蛋白）、培养容器和补料方案支持NK-92细胞扩增、活力和细胞毒性的能力。

结果

NK-92细胞可在含有500 U/mL重组人IL2（普罗白介素）和2.5%人血清/血浆的X-Vivo 10无血清培养基中扩增，以达到足以治疗患者的浓度（>5×10¹⁰细胞）。该方案包括在1 L Vuelife培养袋中以2.5×10⁵细胞/mL接种于25 mL培养基中开始培养，每3天添加新鲜培养基和IL2以维持NK-92细胞扩增的最佳密度。在培养期间每天打散细胞聚集体可增强NK-92细胞的扩增和活力。在符合cGMP的条件下，15 - 17天内最终产量可达到约1.1 - 1.3×10⁶细胞/mL（1.36 - 1.56×10⁹细胞；218 - 250倍扩增），活力>85%。这种方法的可行性已在使用NK-92的正在进行的临床试验中得到证明。