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基因治疗的进展与前景:非病毒载体

Gene therapy progress and prospects: nonviral vectors.

作者信息

Niidome T, Huang L

机构信息

Center for Pharmacogenetics, School of Pharmacy, 633 Salk Hall, University of Pittsburgh, Pittsburgh, PA 15213, USA.

出版信息

Gene Ther. 2002 Dec;9(24):1647-52. doi: 10.1038/sj.gt.3301923.

Abstract

The success of gene therapy is largely dependent on the development of the gene delivery vector. Recently, gene transfection into target cells using naked DNA, which is a simple and safe approach, has been improved by combining several physical techniques, for example, electroporation, gene gun, ultrasound and hydrodynamic pressure. Chemical approaches have been utilized to improve the efficiency and cell specificity of gene transfer. Novel gene carrier molecules, which facilitate DNA escape from the endosome into the cytosol, have been developed. Several functional polymers, which enable controlled release of DNA in response to an environmental change, have also been reported. Plasmids with reduced number of CpG motifs, the use of PCR fragments and the sequential injection method have been established for the reduction of immune response triggered by plasmid DNA. Construction of a long-lasting gene expression system is also an important theme for nonviral gene therapy. To date, tissue-specific expression, self-replicating and integrating plasmid systems have been reported. Improvement of delivery methods together with intelligent design of the DNA itself has brought about large degrees of enhancement in the efficiency, specificity and temporal control of nonviral vectors.

摘要

基因治疗的成功很大程度上取决于基因递送载体的发展。最近,通过结合多种物理技术,如电穿孔、基因枪、超声和流体动力压力,使用裸DNA将基因转染到靶细胞的方法得到了改进,这是一种简单且安全的方法。化学方法已被用于提高基因转移的效率和细胞特异性。已经开发出新型基因载体分子,其有助于DNA从内体逃逸到细胞质中。还报道了几种能够响应环境变化而实现DNA控释的功能聚合物。已经建立了具有减少的CpG基序数量的质粒、使用PCR片段和顺序注射法,以减少由质粒DNA引发的免疫反应。构建持久的基因表达系统也是非病毒基因治疗的一个重要主题。迄今为止,已经报道了组织特异性表达、自我复制和整合质粒系统。递送方法的改进以及DNA本身的智能设计极大地提高了非病毒载体的效率、特异性和时间控制。

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