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阳离子脂质介导的基因传递研究进展:以基于胍基胆固醇的体系为例

Progress in gene delivery by cationic lipids: guanidinium-cholesterol-based systems as an example.

作者信息

Aissaoui Abderrahim, Oudrhiri Noufissa, Petit Laure, Hauchecorne Michelle, Kan Erwan, Sainlos Matthieu, Julia Sébastien, Navarro Jean, Vigneron Jean-Pierre, Lehn Jean-Marie, Lehn Pierre

机构信息

INSERM U458, Hĵpital Robert Debré, Paris, France.

出版信息

Curr Drug Targets. 2002 Feb;3(1):1-16. doi: 10.2174/1389450023348082.

Abstract

Artificial self-assembling systems are currently widely investigated as an alternative approach to recombinant viruses for gene transfection in vitro and in vivo. Cationic lipids are particularly attractive, as a great variety of well-characterized reagents can be synthesized from there. Over the last few years, numerous cationic lipid systems have been developed and shown to be efficient for in vitro transfection. However, although some promising results have been reported in the in vivo setting (even in clinical gene therapy trials in man), the in vivo use of cationic lipid-based systems is still problematic, especially when considering the systemic route of administration. Herein, we summarize our own research on a particular class of cationic lipids, cholesterol derivatives characterized by polar headgroups with guanidinium functions, in order to illustrate the basic principles of and the positive results already obtained by cationic lipid-mediated gene delivery as well as the remaining problems that need to be urgently resolved, particularly as regards the systemic administration. In this forward-looking review, we also discuss the present efforts to develop modular systems for improved in vivo transfection. Indeed, lipid-based vectors offer the possibility to create sophisticated modular gene delivery systems capable of self-assembly via hydrophobic interaction between their components, the role of the different functional elements being to help in overcoming the distinct extracellular and cellular barriers to in vivo gene transfection into the various somatic target tissues.

摘要

目前,人工自组装系统作为重组病毒的替代方法,被广泛研究用于体外和体内基因转染。阳离子脂质尤其具有吸引力,因为可以从它们合成多种特性明确的试剂。在过去几年中,已经开发出许多阳离子脂质系统,并显示出在体外转染方面的高效性。然而,尽管在体内环境中已经报道了一些有前景的结果(甚至在人体临床基因治疗试验中),但基于阳离子脂质的系统在体内的应用仍然存在问题,特别是考虑到全身给药途径时。在此,我们总结了我们自己对一类特定阳离子脂质的研究,这类脂质是以具有胍基功能的极性头基为特征的胆固醇衍生物,以说明阳离子脂质介导的基因递送的基本原理和已经取得的积极成果,以及仍需迫切解决的问题,特别是在全身给药方面。在这篇前瞻性综述中,我们还讨论了目前为开发用于改善体内转染的模块化系统所做的努力。事实上,基于脂质的载体提供了创建复杂模块化基因递送系统的可能性,这些系统能够通过其组分之间的疏水相互作用进行自组装,不同功能元件的作用是帮助克服体内基因转染到各种体细胞靶组织中所面临的不同细胞外和细胞屏障。

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