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针对单纯疱疹病毒感染的人角膜上皮细胞的化学修饰抗病毒 siRNA 群。

Swarms of chemically modified antiviral siRNA targeting herpes simplex virus infection in human corneal epithelial cells.

机构信息

Institute of Biomedicine, University of Turku, Turku, Finland.

Molecular and Integrative Biosciences Research Programme, Faculty of Biological and Environmental Sciences, University of Helsinki, Helsinki, Finland.

出版信息

PLoS Pathog. 2022 Jul 6;18(7):e1010688. doi: 10.1371/journal.ppat.1010688. eCollection 2022 Jul.

Abstract

Herpes simplex virus type 1 (HSV-1) is a common virus of mankind and HSV-1 infections are a significant cause of blindness. The current antiviral treatment of herpes infection relies on acyclovir and related compounds. However, acyclovir resistance emerges especially in the long term prophylactic treatment that is required for prevention of recurrent herpes keratitis. Earlier we have established antiviral siRNA swarms, targeting sequences of essential genes of HSV, as effective means of silencing the replication of HSV in vitro or in vivo. In this study, we show the antiviral efficacy of 2´-fluoro modified antiviral siRNA swarms against HSV-1 in human corneal epithelial cells (HCE). We studied HCE for innate immunity responses to HSV-1, to immunostimulatory cytotoxic double stranded RNA, and to the antiviral siRNA swarms, with or without a viral challenge. The panel of studied innate responses included interferon beta, lambda 1, interferon stimulated gene 54, human myxovirus resistance protein A, human myxovirus resistance protein B, toll-like receptor 3 and interferon kappa. Our results demonstrated that HCE cells are a suitable model to study antiviral RNAi efficacy and safety in vitro. In HCE cells, the antiviral siRNA swarms targeting the HSV UL29 gene and harboring 2´-fluoro modifications, were well tolerated, induced only modest innate immunity responses, and were highly antiviral with more than 99% inhibition of viral release. The antiviral effect of the 2'-fluoro modified swarm was more apparent than that of the unmodified antiviral siRNA swarm. Our results encourage further research in vitro and in vivo on antiviral siRNA swarm therapy of corneal HSV infection, especially with modified siRNA swarms.

摘要

单纯疱疹病毒 1 型(HSV-1)是一种常见的人类病毒,HSV-1 感染是导致失明的重要原因。目前,抗病毒治疗单纯疱疹感染依赖于阿昔洛韦和相关化合物。然而,阿昔洛韦耐药性尤其出现在长期预防性治疗中,这是预防复发性疱疹性角膜炎所必需的。我们之前已经建立了靶向 HSV 必需基因序列的抗病毒 siRNA 群,作为体外或体内沉默 HSV 复制的有效手段。在这项研究中,我们展示了针对 HSV-1 的 2'-氟修饰抗病毒 siRNA 群在人角膜上皮细胞(HCE)中的抗病毒功效。我们研究了 HCE 对 HSV-1 的先天免疫反应、免疫刺激性细胞毒性双链 RNA 以及抗病毒 siRNA 群的反应,有无病毒挑战。所研究的先天反应包括干扰素β、lambda 1、干扰素刺激基因 54、人黏液病毒抗性蛋白 A、人黏液病毒抗性蛋白 B、Toll 样受体 3 和干扰素 kappa。我们的结果表明,HCE 细胞是体外研究抗病毒 RNAi 功效和安全性的合适模型。在 HCE 细胞中,靶向 HSV UL29 基因并携带 2'-氟修饰的抗病毒 siRNA 群耐受性良好,仅诱导适度的先天免疫反应,具有高度抗病毒活性,病毒释放抑制率超过 99%。2'-氟修饰的群的抗病毒效果比未修饰的抗病毒 siRNA 群更为明显。我们的结果鼓励进一步进行体外和体内研究,以开发针对角膜 HSV 感染的抗病毒 siRNA 群治疗方法,特别是使用修饰后的 siRNA 群。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5201/9292126/c8aa0eb38495/ppat.1010688.g001.jpg

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