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Adenovirus vectors lacking virus-associated RNA expression enhance shRNA activity to suppress hepatitis C virus replication

机译:缺乏病毒相关RNA表达的腺病毒载体可增强shRNA活性以抑制丙型肝炎病毒复制

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First-generation adenovirus vectors (FG AdVs) expressing short-hairpin RNA (shRNA) effectively downregulate the expressions of target genes. However, this vector, in fact, expresses not only the transgene product, but also virus-associated RNAs (VA RNAs) that disturb cellular RNAi machinery. We have established a production method for VA-deleted AdVs lacking expression of VA RNAs. Here, we showed that the highest shRNA activity was obtained when the shRNA was inserted not at the popularly used E1 site, but at the E4 site. We then compared the activities of shRNAs against hepatitis C virus (HCV) expressed from VA-deleted AdVs or conventional AdVs. The VA-deleted AdVs inhibited HCV production much more efficiently. Therefore, VA-deleted AdVs were more effective than the currently used AdVs for shRNA downregulation, probably because of the lack of competition between VA RNAs and the shRNAs. These VA-deleted AdVs might enable more effective gene therapies for chronic hepatitis C.
机译:表达短发夹RNA(shRNA)的第一代腺病毒载体(FG AdVs)有效下调靶基因的表达。但是,实际上,该载体不仅表达转基因产物,而且表达干扰细胞RNAi机制的病毒相关RNA(VA RNA)。我们已经建立了缺失VA RNA的VA缺失AdV的生产方法。在这里,我们显示了将shRNA插入到不是普遍使用的E1位点,而是插入到E4位点时可获得最高的shRNA活性。然后,我们比较了从VA缺失的AdV或常规AdV表达的shRNA对抗丙型肝炎病毒(HCV)的活性。 VA缺失的AdVs更有效地抑制HCV产生。因此,VA缺失的AdV对shRNA下调的作用比目前使用的AdV更有效,这可能是因为VA RNA与shRNA之间缺乏竞争。这些VA缺失的AdV可能会为慢性丙型肝炎提供更有效的基因治疗。

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