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RNA干扰在哺乳动物系统中的最新应用。

Recent applications of RNAi in mammalian systems.

作者信息

Scherer Lisa, Rossi John J

机构信息

Division of Molecular Biology, Beckman Research Institute of the City of Hope, Duarte, CA 91010, USA.

出版信息

Curr Pharm Biotechnol. 2004 Aug;5(4):355-60. doi: 10.2174/1389201043376724.

Abstract

RNAi is a powerful cellular mechanism that involves targeted destruction of mRNAs. Although the phenomenon was first discovered in plants and lower eukaryotic organisms, it was later discovered as an important genetic regulatory mechanism in mammalian cells. RNAi is triggered by double stranded RNAs that are cleaved into short 21-23 base pair duplexes by an RNAse III type enzyme called Dicer. The short RNAs, termed small interfering RNAs (siRNAs), act as triggers for targeted RNA degradation. One of the two strands is selectively incorporated into a complex of proteins called the RNA induced silencing complex, or RISC. The incorporated small RNA guides the complex to the complementary target sequence, and this event is followed by endonucleolytic cleavage of the target and recycling of RISC. In mammalian cells, siRNAs do not activate interferon pathway genes, thereby making these powerful tools for sequence specific knockdown of RNAs. In this article we review the methods for programming mammalian cells with siRNAs, and overview a number of applications ranging from targeting oncogenes to inhibiting viral replication. The article also summarizes some important biological conclusions that can be drawn from selective downregulation of certain mRNA targets and addresses potential uses of RNAi as a new therapeutic modality.

摘要

RNA干扰是一种强大的细胞机制,涉及对信使核糖核酸(mRNA)的靶向破坏。尽管这一现象最初是在植物和低等真核生物中发现的,但后来被发现是哺乳动物细胞中的一种重要基因调控机制。RNA干扰由双链RNA触发,双链RNA被一种名为Dicer的核糖核酸酶III型酶切割成短的21 - 23个碱基对的双链体。这些短RNA,称为小干扰RNA(siRNA),作为靶向RNA降解的触发因素。两条链中的一条被选择性地整合到一种名为RNA诱导沉默复合体(RISC)的蛋白质复合物中。整合的小RNA引导该复合物找到互补的靶序列,随后靶标被核酸内切酶切割,RISC循环利用。在哺乳动物细胞中,小干扰RNA不会激活干扰素途径基因,因此这些强大的工具可用于对RNA进行序列特异性敲低。在本文中,我们回顾了用小干扰RNA对哺乳动物细胞进行编程的方法,并概述了从靶向癌基因到抑制病毒复制等一系列应用。本文还总结了一些可以从某些mRNA靶标的选择性下调中得出的重要生物学结论,并探讨了RNA干扰作为一种新的治疗方式的潜在用途。

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