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Attenuation of vesicular stomatitis virus infection of brain using antiviral drugs and an adeno-associated virus-interferon vector

机译:使用抗病毒药物和腺相关病毒-干扰素载体减轻脑水泡性口炎病毒感染

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Vesicular stomatitis virus (VSV) shows promise as a vaccine-vector and oncolytic virus. However, reports of neurotoxicity of VSV remain a concern. We compared 12 antiviral compounds to control infection of VSV-CT9-M51 and VSV-rp30 using murine and human brain cultures, and in vivo mouse models. Inhibition of replication, cytotoxicity and infectivity was strongest with ribavirin and IFN-alpha and to some extent with mycophenolic acid, chloroquine, and adenine 9-beta-D-arabinofuranoside. To generate continuous IFN exposure, we made an adeno-associated virus vector expressing murine IFN; AAV-mIFN-beta protected mouse brain cells from VSV, as did a combination of IFN, ribavirin and chloroquine. Intracranial AAV-mIFN-beta protected the brain against VSV-CT9-M51. In SCID mice bearing human glioblastoma, AAV-mIFN-beta moderately enhanced survival. VSV-CT9-M51 doubled median survival when administered after AAV-mIFN-beta; some surviving mice showed complete tumor destruction. Together, these data suggest that AAV-IFN or IFN with ribavirin and chloroquine provide an optimal anti-virus combination against VSV in the brain. (C) 2014 Elsevier Inc. All rights reserved.
机译:水泡性口炎病毒(VSV)有望作为疫苗载体和溶瘤病毒。然而,关于VSV的神经毒性的报道仍然令人关注。我们比较了12种抗病毒化合物使用鼠和人脑培养物以及体内小鼠模型来控制VSV-CT9-M51和VSV-rp30的感染。利巴韦林和IFN-α对复制,细胞毒性和感染性的抑制作用最强,在一定程度上对麦考酚酸,氯喹和腺嘌呤9-β-D-阿拉伯呋喃糖苷具有抑制作用。为了产生连续的IFN暴露,我们制备了表达鼠IFN的腺相关病毒载体。 AAV-mIFN-β与IFN,利巴韦林和氯喹的组合一样,可以保护小鼠脑细胞免受VSV侵害。颅内AAV-mIFN-β保护大脑免受VSV-CT9-M51的侵害。在携带人胶质母细胞瘤的SCID小鼠中,AAV-mIFN-β适度提高了存活率。在AAV-mIFN-beta给药后,VSV-CT9-M51的中位生存时间增加了一倍;一些存活的小鼠显示出完全的肿瘤破坏。总之,这些数据表明,AAV-IFN或IFN与利巴韦林和氯喹提供了针对脑中VSV的最佳抗病毒组合。 (C)2014 Elsevier Inc.保留所有权利。

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