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逆转录病毒载体的整合位点选择:分子机制与临床后果

Integration site selection by retroviral vectors: molecular mechanism and clinical consequences.

作者信息

Daniel René, Smith Johanna A

机构信息

Division of Infectious Diseases, Center for Human Virology, Kimmel Cancer Center, Thomas Jefferson University, Philadelphia, PA 19107, USA.

出版信息

Hum Gene Ther. 2008 Jun;19(6):557-68. doi: 10.1089/hum.2007.148.

Abstract

Retroviral DNA integration into the host cell genome is an essential feature of the retroviral life cycle. The ability to integrate their DNA into the DNA of infected cells also makes retroviruses attractive vectors for delivery of therapeutic genes into the genome of cells carrying adverse mutations in their cellular DNA. Sequencing of the entire human genome has enabled identification of integration site preferences of both replication-competent retroviruses and retroviral vectors. These results, together with the unfortunate outcome of a gene therapy trial, in which integration of a retroviral vector in the vicinity of a protooncogene was associated with the development of leukemia, have stimulated efforts to elucidate the molecular mechanism underlying integration site selection by retroviral vectors, as well as the development of methods to direct integration to specific DNA sequences and chromosomal regions. This review outlines our current knowledge of the mechanism of integration site selection by retroviruses in vitro, in cultured cells, and in vivo; the outcome of several of the more recent gene therapy trials, which employed these vectors; and the efforts of several laboratories to develop vectors that integrate at predetermined sites in the human genome.

摘要

逆转录病毒DNA整合到宿主细胞基因组是逆转录病毒生命周期的一个基本特征。将其DNA整合到受感染细胞的DNA中的能力也使逆转录病毒成为有吸引力的载体,可用于将治疗性基因递送到细胞DNA中携带有害突变的细胞基因组中。对整个人类基因组进行测序,已能够确定有复制能力的逆转录病毒和逆转录病毒载体的整合位点偏好。这些结果,再加上一项基因治疗试验的不幸结果(在该试验中,逆转录病毒载体在原癌基因附近的整合与白血病的发生有关),促使人们努力阐明逆转录病毒载体选择整合位点的分子机制,以及开发将整合定向到特定DNA序列和染色体区域的方法。本综述概述了我们目前对逆转录病毒在体外、培养细胞和体内选择整合位点机制的了解;采用这些载体的一些最新基因治疗试验的结果;以及几个实验室为开发能整合到人类基因组预定位点的载体所做的努力。

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