基因修饰干细胞在腺苷脱氨酶缺乏性免疫缺陷中的临床疗效
Clinical efficacy of gene-modified stem cells in adenosine deaminase-deficient immunodeficiency.
作者信息
Shaw Kit L, Garabedian Elizabeth, Mishra Suparna, Barman Provaboti, Davila Alejandra, Carbonaro Denise, Shupien Sally, Silvin Christopher, Geiger Sabine, Nowicki Barbara, Smogorzewska E Monika, Brown Berkley, Wang Xiaoyan, de Oliveira Satiro, Choi Yeong, Ikeda Alan, Terrazas Dayna, Fu Pei-Yu, Yu Allen, Fernandez Beatriz Campo, Cooper Aaron R, Engel Barbara, Podsakoff Greg, Balamurugan Arumugam, Anderson Stacie, Muul Linda, Jagadeesh G Jayashree, Kapoor Neena, Tse John, Moore Theodore B, Purdy Ken, Rishi Radha, Mohan Kathey, Skoda-Smith Suzanne, Buchbinder David, Abraham Roshini S, Scharenberg Andrew, Yang Otto O, Cornetta Kenneth, Gjertson David, Hershfield Michael, Sokolic Rob, Candotti Fabio, Kohn Donald B
出版信息
J Clin Invest. 2017 May 1;127(5):1689-1699. doi: 10.1172/JCI90367. Epub 2017 Mar 27.
BACKGROUND
Autologous hematopoietic stem cell transplantation (HSCT) of gene-modified cells is an alternative to enzyme replacement therapy (ERT) and allogeneic HSCT that has shown clinical benefit for adenosine deaminase-deficient (ADA-deficient) SCID when combined with reduced intensity conditioning (RIC) and ERT cessation. Clinical safety and therapeutic efficacy were evaluated in a phase II study.
METHODS
Ten subjects with confirmed ADA-deficient SCID and no available matched sibling or family donor were enrolled between 2009 and 2012 and received transplantation with autologous hematopoietic CD34+ cells that were modified with the human ADA cDNA (MND-ADA) γ-retroviral vector after conditioning with busulfan (90 mg/m2) and ERT cessation. Subjects were followed from 33 to 84 months at the time of data analysis. Safety of the procedure was assessed by recording the number of adverse events. Efficacy was assessed by measuring engraftment of gene-modified hematopoietic stem/progenitor cells, ADA gene expression, and immune reconstitution.
RESULTS
With the exception of the oldest subject (15 years old at enrollment), all subjects remained off ERT with normalized peripheral blood mononuclear cell (PBMC) ADA activity, improved lymphocyte numbers, and normal proliferative responses to mitogens. Three of nine subjects were able to discontinue intravenous immunoglobulin replacement therapy. The MND-ADA vector was persistently detected in PBMCs (vector copy number [VCN] = 0.1-2.6) and granulocytes (VCN = 0.01-0.3) through the most recent visits at the time of this writing. No patient has developed a leukoproliferative disorder or other vector-related clinical complication since transplant.
CONCLUSION
These results demonstrate clinical therapeutic efficacy from gene therapy for ADA-deficient SCID, with an excellent clinical safety profile.
TRIAL REGISTRATION
ClinicalTrials.gov NCT00794508.
FUNDING
Food and Drug Administration Office of Orphan Product Development award, RO1 FD003005; NHLBI awards, PO1 HL73104 and Z01 HG000122; UCLA Clinical and Translational Science Institute awards, UL1RR033176 and UL1TR000124.
背景
基因修饰细胞的自体造血干细胞移植(HSCT)是酶替代疗法(ERT)和异基因HSCT的一种替代方法,当与降低强度预处理(RIC)和停止ERT联合使用时,已显示出对腺苷脱氨酶缺乏(ADA缺乏)的重症联合免疫缺陷(SCID)有临床益处。在一项II期研究中评估了临床安全性和治疗效果。
方法
2009年至2012年期间,招募了10名确诊为ADA缺乏SCID且没有匹配的同胞或家族供体的受试者,在接受白消安(90 mg/m2)预处理并停止ERT后,接受用人ADA cDNA(MND-ADA)γ逆转录病毒载体修饰的自体造血CD34+细胞移植。在数据分析时,对受试者进行了33至84个月的随访。通过记录不良事件的数量来评估该程序的安全性。通过测量基因修饰的造血干/祖细胞的植入、ADA基因表达和免疫重建来评估疗效。
结果
除最年长的受试者(入组时15岁)外,所有受试者均停止ERT,外周血单核细胞(PBMC)ADA活性正常化,淋巴细胞数量增加,对有丝分裂原的增殖反应正常。9名受试者中有3名能够停止静脉注射免疫球蛋白替代疗法。在撰写本文时,通过最近的随访,在PBMC(载体拷贝数[VCN]=0.1-2.6)和粒细胞(VCN=0.01-0.3)中持续检测到MND-ADA载体。自移植以来,没有患者发生白细胞增殖性疾病或其他与载体相关的临床并发症。
结论
这些结果证明了基因治疗对ADA缺乏SCID的临床治疗效果,具有出色的临床安全性。
试验注册
ClinicalTrials.gov NCT00794508。
资助
美国食品药品监督管理局孤儿产品开发办公室奖,RO1 FD003005;美国国立心肺血液研究所奖,PO1 HL73104和Z01 HG000122;加州大学洛杉矶分校临床与转化科学研究所奖,UL1RR033176和UL1TR000124。
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