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RNA interference in vitro and in vivo using DsiRNA targeting the nucleocapsid N mRNA of human metapneumovirus

机译:使用靶向人间质肺病毒的核衣壳N mRNA的DsiRNA进行体内外RNA干扰

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Human metapneumovirus causes respiratory diseases with outcomes that can be severe in children, the immunocompromised, and the elderly. Synthetic small interfering RNAs (siRNAs) that silence targeted genes can be used as therapeutic agents. Currently, there is no specific therapy for hMPV. In this study, we designed Dicer-substrate siRNAs (DsiRNAs) that target metapneumovirus sequences on the mRNAs of the N, P, and L genes. In vitro, six DsiRNAs were shown to inhibit virus replication using cell proliferation tests. Of those, the DsiRNA that targets the most conserved mRNA sequence was then resynthesized in Evader? format with heavy 2'-O-methyl modification of the guide strand. In a murine model, the prophylactic administration of this Evader? DsiRNA was effective at partially inhibiting viral replication of hMPV (13×10 3 vs. 29×10 3PFU/g of lung; p0.01), which was not the case for the control, a mismatched DsiRNA. Inhibition was achieved without inducing cytokines or off-target effects. Moreover, the specificity of the siRNA mechanism of action was demonstrated in vitro and in vivo using 5'-RACE methodology. This in vivo approach of using a DsiRNA against hMPV is an important step in the development of synthetic siRNA as a therapeutic agent for this virus.
机译:人间质肺炎病毒会导致呼吸道疾病,其后果在儿童,免疫功能低下和老年人中可能很严重。使靶基因沉默的合成小干扰RNA(siRNA)可用作治疗剂。当前,没有针对hMPV的特异性疗法。在这项研究中,我们设计了切丁酶底物siRNA(DsiRNA),其靶向N,P和L基因的mRNA上的偏肺病毒序列。在体外,使用细胞增殖测试显示六个DsiRNA可抑制病毒复制。其中,靶向最保守的mRNA序列的DsiRNA然后在Evader?中重新合成。引导链的2'-O-甲基进行了重修饰。在鼠模型中,该Evader的预防性给药是? DsiRNA可有效部分抑制hMPV的病毒复制(13×10 3 vs. 29×10 3PFU / g肺; p <0.01),而对照品(错配的DsiRNA)则并非如此。在不诱导细胞因子或脱靶效应的情况下实现了抑制作用。而且,使用5'-RACE方法在体外和体内证明了siRNA作用机制的特异性。使用针对hMPV的DsiRNA的这种体内方法是开发合成siRNA作为该病毒治疗剂的重要一步。

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