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用于体内基因递送的非病毒载体:物理化学和药代动力学考量

Nonviral vectors for in vivo gene delivery: physicochemical and pharmacokinetic considerations.

作者信息

Mahato R I, Takakura Y, Hashida M

机构信息

Department of Drug Delivery Research, Faculty of Pharmaceutical Sciences, Kyoto University, Japan.

出版信息

Crit Rev Ther Drug Carrier Syst. 1997;14(2):133-72.

PMID:9107520
Abstract

The use of nonviral vectors is an attractive in vivo gene delivery strategy that is simpler than, and lacks some risks inherent in, viral systems. Liposomes and receptor-mediated polycation systems are promising carriers for delivery and expression of plasmid DNA encoding genes into the target cells. Many barriers need to be overcome for successful in vivo DNA delivery using these carrier systems. Such factors as extent of DNA condensation, particle size of the DNA complex, route of administration, stability against nucleases, target sites, in vivo disposition, binding to cell surface receptor and internalization, and intracellular trafficking affect in vivo gene delivery and expression. This review will provide a critical discussion of the merits and limitations of liposomal and polycationic carrier systems for gene transfer from the viewpoints of their physicochemical and pharmacokinetic properties.

摘要

使用非病毒载体是一种有吸引力的体内基因递送策略,它比病毒系统更简单,且不存在病毒系统固有的一些风险。脂质体和受体介导的聚阳离子系统是将编码基因的质粒DNA递送至靶细胞并实现表达的有前景的载体。要使用这些载体系统成功进行体内DNA递送,需要克服许多障碍。诸如DNA凝聚程度、DNA复合物的粒径、给药途径、对核酸酶的稳定性、靶位点、体内处置、与细胞表面受体的结合及内化以及细胞内运输等因素都会影响体内基因递送和表达。本综述将从脂质体和聚阳离子载体系统的物理化学和药代动力学特性的角度,对其在基因转移方面的优缺点进行批判性讨论。

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