首页> 美国卫生研究院文献>Nucleic Acids Research >Antiviral activity and possible mechanisms of action of oligonucleotides-poly(L-lysine) conjugates targeted to vesicular stomatitis virus mRNA and genomic RNA.
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Antiviral activity and possible mechanisms of action of oligonucleotides-poly(L-lysine) conjugates targeted to vesicular stomatitis virus mRNA and genomic RNA.

机译:靶向水疱​​性口炎病毒mRNA和基因组RNA的寡核苷酸-聚(L-赖氨酸)缀合物的抗病毒活性和可能的​​作用机理。

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摘要

Synthetic oligonucleotides (oligomers) complementary to vesicular stomatitis virus (VSV) N protein mRNA have specific antiviral properties at concentrations lower than 1 microM when they are covalently linked to poly(L-lysine) (PLL). Since it is generally postulated that antisense oligomers act at the translational level, oligomers with potential targets on VSV viral mRNA and/or genomic RNA have been tested here. In vitro translation experiments in reticulocyte lysates, in vitro transcription experiments with permeabilized viruses, measurement of viral RNA transcription and accumulation in VSV infected cells, and antiviral experiments demonstrate in our model that antisense oligomers probably also act at other levels. Difficulties in the choice of the most effective antisense oligomer targets are also discussed.
机译:当与聚(L-赖氨酸)(PLL)共价连接时,与水泡性口腔炎病毒(VSV)N蛋白mRNA互补的合成寡核苷酸(寡聚物)在低于1 microM的浓度下具有特定的抗病毒特性。由于通常假定反义寡聚体在翻译水平起作用,因此在此已经测试了对VSV病毒mRNA和/或基因组RNA具有潜在靶标的寡聚体。网织红细胞裂解物的体外翻译实验,通透性病毒的体外转录实验,VSV感染细胞中病毒RNA转录和积累的测量以及抗病毒实验在我们的模型中证明,反义寡聚体也可能在其他水平上起作用。还讨论了选择最有效的反义低聚物靶标的困难。

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