利用靶向和稳定的纳米颗粒克服白细胞中的RNAi转导。

Idrugs Pub Date : 2010-09-01
Rofa Elfakess, Dan Peer
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引用次数: 0

摘要

基于rnai的方法为提高对基因在体外表达和功能的理解做出了重大贡献。在体内应用这些策略来验证特定基因在正常或病理条件下的作用,并诱导基因沉默的能力,为使用RNAi作为一种新的治疗方式带来了新的可能性。然而,RNAi从一种有效的基因组工具转化为临床应用一直受到RNAi分子通过全身给药递送到靶组织(特别是造血细胞)的挑战的阻碍。本专题综述描述了目前针对白细胞的系统性RNAi递送平台,重点关注整合素靶向稳定纳米颗粒策略,该策略使用白细胞整合素将sirna专门递送到免疫系统细胞。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Overcoming RNAi transduction in leukocytes using targeted and stabilized nanoparticles.

RNAi-based approaches have contributed significantly to the improved understanding of gene expression and function in vitro. The ability to apply these strategies in vivo to validate the role of specific genes in normal or pathological conditions, and to induce gene silencing, has led to new possibilities for using RNAi as a novel therapeutic modality. However, the translation of RNAi from an effective genomic tool into clinical applications has been hindered by the challenge of delivering RNAi molecules to their target tissues by systemic administration, particularly to hematopoietic cells. This feature review describes the current systemic RNAi delivery platforms targeted to leukocytes, with a focus on the integrin-targeted stabilized nanoparticles strategy, which uses leukocyte integrins for the delivery of siRNAs exclusively to cells of the immune system.

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来源期刊
Idrugs
Idrugs 医学-药学
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