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利用双链RNA预防重组杆状病毒在体外和体内的病毒感染。

Using double-stranded RNA to prevent in vitro and in vivo viral infections by recombinant baculovirus.

作者信息

Valdes Victor Julian, Sampieri Alicia, Sepulveda Jorge, Vaca Luis

机构信息

Departamento de Biología Celular, Instituto de Fisiología Celular, Universidad Nacional Autonoma de Mexico, México City DF 04510, Mexico.

出版信息

J Biol Chem. 2003 May 23;278(21):19317-24. doi: 10.1074/jbc.M212039200. Epub 2003 Mar 19.

Abstract

Introduction of double-stranded RNA (dsRNA) into a wide variety of cells and organisms results in post-transcriptional depletion of the homologue endogenous mRNA. This well-preserved phenomenon known as RNA interference (RNAi) is present in evolutionarily diverse organisms such as plants, fungi, insects, metazoans, and mammals. Because the identification of the targeted mRNA by the RNAi machinery depends upon Watson-Crick base-pairing interactions, RNAi can be exquisitely specific. We took advantage of this powerful and flexible technique to demonstrate that selective silencing of genes essential for viral propagation prevents in vitro and in vivo viral infection. Using the baculovirus Autographa californica, a rapidly replicating and highly cytolytic double-stranded DNA virus that infects many different insect species, we show for the first time that introduction of dsRNA from gp64 and ie1, two genes essential for baculovirus propagation, results in prevention of viral infection in vitro and in vivo. This is the first report demonstrating the use of RNAi to inhibit a viral infection in animals. This inhibition was specific, because dsRNA from the polyhedrin promoter (used as control) or unrelated dsRNAs did not affect the time course of viral infection. The most relevant consequences from the present study are: 1) RNAi offers a rapid and efficient way to interfere with viral genes to assess the role of specific proteins in viral function and 2) using RNAi to interfere with viral genes essential for cell infection may provide a powerful therapeutic tool for the treatment of viral infections.

摘要

将双链RNA(dsRNA)导入多种细胞和生物体中会导致同源内源性mRNA在转录后减少。这种保存完好的现象被称为RNA干扰(RNAi),存在于植物、真菌、昆虫、后生动物和哺乳动物等进化上不同的生物体中。由于RNAi机制对靶向mRNA的识别依赖于沃森-克里克碱基配对相互作用,RNAi可以具有高度特异性。我们利用这种强大且灵活的技术证明,对病毒繁殖所必需的基因进行选择性沉默可预防体外和体内的病毒感染。使用苜蓿银纹夜蛾核型多角体病毒,一种快速复制且具有高度细胞溶解性的双链DNA病毒,可感染许多不同的昆虫物种,我们首次表明,导入来自gp64和ie1(苜蓿银纹夜蛾核型多角体病毒繁殖所必需的两个基因)的dsRNA可预防体外和体内的病毒感染。这是第一份证明使用RNAi抑制动物病毒感染的报告。这种抑制是特异性的,因为来自多角体蛋白启动子的dsRNA(用作对照)或无关的dsRNA不影响病毒感染的时间进程。本研究最相关的结果是:1)RNAi提供了一种快速有效的方法来干扰病毒基因,以评估特定蛋白质在病毒功能中的作用;2)使用RNAi干扰细胞感染所必需的病毒基因可能为治疗病毒感染提供一种强大的治疗工具。

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