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通过致死性诱变对RNA病毒进行治疗性靶向。

Therapeutically targeting RNA viruses via lethal mutagenesis.

作者信息

Graci Jason D, Cameron Craig E

机构信息

PTC Therapeutics, Inc., 100 Corporate Court, South Plainfield, NJ 07080, USA, Tel.: +1 908 912 9249; ;

出版信息

Future Virol. 2008 Nov;3(6):553-566. doi: 10.2217/17460794.3.6.553.

Abstract

RNA viruses exhibit increased mutation frequencies relative to other organisms. Recent work has attempted to exploit this unique feature by increasing the viral mutation frequency beyond an extinction threshold, an antiviral strategy known as lethal mutagenesis. A number of novel nucleoside analogs have been designed around this premise. Herein, we review the quasispecies nature of RNA viruses and survey the antiviral, biological and biochemical characteristics of mutagenic nucleoside analogs, including clinically-used ribavirin. Biological implications of modulating viral replication fidelity are discussed in the context of translating lethal mutagenesis into a clinically-useful antiviral strategy.

摘要

与其他生物体相比,RNA病毒表现出更高的突变频率。最近的研究试图利用这一独特特征,将病毒突变频率提高到灭绝阈值以上,这是一种被称为致死诱变的抗病毒策略。基于这一前提,人们设计了许多新型核苷类似物。在此,我们综述了RNA病毒的准种性质,并考察了诱变核苷类似物的抗病毒、生物学和生化特性,包括临床使用的利巴韦林。在将致死诱变转化为临床有用的抗病毒策略的背景下,讨论了调节病毒复制保真度的生物学意义。

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