Felsburg Peter J, De Ravin Suk See, Malech Harry L, Sorrentino Brian P, Burtner Christopher, Kiem Hans-Peter
1 Department of Clinical Studies, School of Veterinary Medicine, University of Pennsylvania , Philadelphia, PA 19104.
Hum Gene Ther Clin Dev. 2015 Mar;26(1):50-6. doi: 10.1089/humc.2015.004. Epub 2015 Feb 24.
Since the occurrence of T cell leukemias in the original human γ-retroviral gene therapy trials for X-linked severe combined immunodeficiency (XSCID), considerable effort has been devoted to developing safer vectors. This review summarizes gene therapy studies performed in a canine model of XSCID to evaluate the efficacy of γ-retroviral, lentiviral, and foamy viral vectors for treating XSCID and a novel method of vector delivery. These studies demonstrate that durable T cell reconstitution and thymopoiesis with no evidence of any serious adverse events and, in contrast to the human XSCID patients, sustained marking in myeloid cells and B cells with reconstitution of normal humoral immune function can be achieved for up to 5 years without any pretreatment conditioning. The presence of sustained levels of gene-marked T cells, B cells, and more importantly myeloid cells for almost 5 years is highly suggestive of transduction of either multipotent hematopoietic stem cells or very primitive committed progenitors.
自从在最初针对X连锁重症联合免疫缺陷病(XSCID)的人类γ逆转录病毒基因治疗试验中出现T细胞白血病以来,人们投入了大量精力来开发更安全的载体。本综述总结了在XSCID犬模型中进行的基因治疗研究,以评估γ逆转录病毒、慢病毒和泡沫病毒载体治疗XSCID的疗效以及一种新型载体递送方法。这些研究表明,可实现持久的T细胞重建和胸腺生成,且无任何严重不良事件的证据,与人类XSCID患者不同,无需任何预处理条件,正常体液免疫功能重建的髓系细胞和B细胞可持续标记长达5年。持续近5年的基因标记T细胞、B细胞,更重要的是髓系细胞的存在,强烈提示多能造血干细胞或非常原始的定向祖细胞发生了转导。
