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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Current developments in the design of onco-retrovirus and lentivirus vector systems for hematopoietic cell gene therapy
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Current developments in the design of onco-retrovirus and lentivirus vector systems for hematopoietic cell gene therapy

机译:用于造血细胞基因治疗的癌逆转录病毒和慢病毒载体系统设计的最新进展

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Over the past dozen years, the majority of clinical gene therapy trials for inherited genetic diseases and cancer therapy have been performed using murine onco-retrovirus as the gene delivery vector. The earliest systems used were relatively inefficient in both the rates of transduction and expression of the transgene. Formidable obstacles inherent in the cell biology and/or the immunology of the target cell systems limited the efficacy of gene therapy for many target diseases. Development of novel retrovirus gene transfer systems that are in progress have begun to overcome these obstacles. Evidence of this progress is the recent successful functional correction of the immune T and B lymphocyte deficiency in patients with X-linked severe combined immunodeficiency (X-SCID) and adenosine deaminase (ADA)-deficient SCID following once-retrovirus vector ex vivo transduction of autologous marrow stem cells [Science 296 (2002) 2410; Science 288 (2000) 669; N. Engl. J. Med. 346 (2002) 1185]. These achievements of prolonged clinical benefit from gene therapy were tempered by the finding of insertional mutageneses in two of the treated X-SCID patients [N. Engl. J. Med. 348 (2003) 255].
机译:在过去的十几年中,大多数关于遗传性遗传疾病和癌症治疗的临床基因治疗试验都是使用鼠类逆转录病毒作为基因传递载体进行的。最早使用的系统在转导率和转基因表达方面均相对低效。在靶细胞系统的细胞生物学和/或免疫学中固有的强大障碍限制了基因治疗对许多靶疾病的功效。正在进行的新型逆转录病毒基因转移系统的开发已开始克服这些障碍。取得这一进展的证据是最近一次逆转录病毒载体离体转导X连锁严重联合免疫缺陷(X-SCID)和腺苷脱氨酶(ADA)缺陷的SCID患者的免疫T和B淋巴细胞缺乏症的近期成功的功能校正。自体骨髓干细胞[Science 296(2002)2410;科学288(2000)669; N. Engl。 J. Med。 346(2002)1185]。在两名接受治疗的X-SCID患者中发现了插入突变,从而减轻了基因治疗延长临床获益的这些成就[N. Engl。 J. Med。 348(2003)255]。

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