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Adenovirus-mediated artificial MicroRNAs targeting matrix or nucleoprotein genes protect mice against lethal influenza virus challenge

机译:靶向基质或核蛋白基因的腺病毒介导的人工MicroRNA保护小鼠抵抗致命的流感病毒攻击

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摘要

Influenza virus (IV) infection is a major public health problem, causing millions of cases of severe illness and as many as 500 000 deaths each year worldwide. Given the limitations of current prevention or treatment of acute influenza, novel therapies are needed. RNA interference (RNAi) through microRNAs (miRNA) is an emerging technology that can suppress virus replication in vitro and in vivo. Here, we describe a novel strategy for the treatment of infuenza based on RNAi delivered by a replication-defective adenovirus (Ad) vector, derived from chimpanzee serotype 68 (AdC68). Our results showed that artificial miRNAs (amiRNAs) specifically targeting conserved regions of the IV genome could effectively inhibit virus replication in human embryonic kidney 293 cells. Moreover, our results demonstrated that prophylactic treatment with AdC68 expressing amiRNAs directed against M1, M2 or nucleoprotein genes of IV completely protected mice from homologous A/PR8 virus challenge and partially protected the mice from heterologous influenza A virus strains such as H9N2 and H5N1. Collectively, our data demonstrate that amiRNAs targeting the conserved regions of influenza A virus delivered by Ad vectors should be pursued as a novel strategy for prophylaxis of IV infection in humans and animals.
机译:流感病毒(IV)感染是主要的公共卫生问题,全世界每年造成数百万例严重疾病,并有50万人死亡。考虑到当前预防或治疗急性流感的局限性,需要新的疗法。通过微RNA(miRNA)进行RNA干扰(RNAi)是一种新兴技术,可以抑制病毒在体外和体内的复制。在这里,我们描述了一种基于RNAi的新型流感治疗策略,该RNAi由源自黑猩猩血清型68(AdC68)的复制缺陷型腺病毒(Ad)载体提供。我们的结果表明,专门针对IV基因组保守区域的人工miRNA(amiRNA)可以有效抑制人胚胎肾293细胞中的病毒复制。此外,我们的结果表明,用针对Ad的M1,M2或IV核蛋白基因的表达AdC68的amiRNA进行的预防性处理完全保护了小鼠免受同源A / PR8病毒的攻击,并部分保护了小鼠免受异源甲型流感病毒株(如H9N2和H5N1)的侵害。总体而言,我们的数据表明,应采用靶向Ad载体递送的A型流感病毒保守区的amiRNA作为预防人和动物IV感染的新策略。

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