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用鼻内小干扰RNA治疗呼吸道病毒感染。

Therapy of respiratory viral infections with intranasal siRNAs.

作者信息

Barik Sailen, Lu Patrick

机构信息

Center for Gene Regulation in Health and Disease, Cleveland State University, Cleveland, OH, USA,

出版信息

Methods Mol Biol. 2015;1218:251-62. doi: 10.1007/978-1-4939-1538-5_14.

Abstract

Chemically synthesized short interfering RNA (siRNA) has ushered a new era in the application of RNA interference (RNAi) against viral genes. We have paid particular attention to respiratory viruses that wreak heavy morbidity and mortality worldwide. The clinically significant ones include respiratory syncytial virus (RSV), parainfluenza virus (PIV) (two Paramyxoviruses), and influenza virus (an Orthomyxovirus). As the infection by these viruses is clinically restricted to the respiratory tissues, mainly the lungs, the logical route for the application of the siRNA was also the same, i.e., via the nasal route. Following the initial success of single intranasal siRNA against RSV, we now offer two new strategies: (1) second-generation siRNAs, used against the paramyxoviral RNA polymerase large subunit (L), (2) siRNA cocktail with a novel transfection reagent, used against influenza virus. Based on these results, we propose the following consensus for designing intranasal antiviral siRNAs: (a) modified 19-27 nt-long double-stranded siRNAs are functional in the lung, (b) excessive 2'-OMe and 2'-F modifications in either or both strands of these siRNAs reduce efficacy, (c) limited modifications in the sense strand are beneficial, although their precise efficacy may be position-dependent, (d) cocktail of multiple siRNAs can be highly effective against multiple viral strains and subtypes.

摘要

化学合成的短干扰RNA(siRNA)开启了RNA干扰(RNAi)应用于抗病毒基因的新时代。我们特别关注在全球造成严重发病和死亡的呼吸道病毒。具有临床意义的病毒包括呼吸道合胞病毒(RSV)、副流感病毒(PIV)(两种副粘病毒)和流感病毒(一种正粘病毒)。由于这些病毒的感染在临床上局限于呼吸道组织,主要是肺部,因此应用siRNA的合理途径也是相同的,即通过鼻腔途径。在单次鼻内给予siRNA对抗RSV取得初步成功之后,我们现在提供两种新策略:(1)用于对抗副粘病毒RNA聚合酶大亚基(L)的第二代siRNA,(2)与新型转染试剂联用的siRNA混合物,用于对抗流感病毒。基于这些结果,我们提出以下关于设计鼻内抗病毒siRNA的共识:(a)19 - 27个核苷酸长的经修饰双链siRNA在肺部具有功能,(b)这些siRNA的一条链或两条链中过量的2'-O-甲基和2'-氟修饰会降低疗效,(c)正义链中的有限修饰是有益的,尽管其确切疗效可能取决于位置,(d)多种siRNA的混合物对多种病毒株和亚型可能非常有效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1f8f/7122875/b572ea79917b/316107_1_En_14_Fig1_HTML.jpg

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