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使用抗病毒药物和腺相关病毒-干扰素载体减轻脑内水泡性口炎病毒感染

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

作者信息

Wollmann Guido, Paglino Justin C, Maloney Patrick R, Ahmadi Sebastian A, van den Pol Anthony N

机构信息

Department of Neurosurgery, Yale University School of Medicine, New Haven, CT 06520, United States.

Department of Neurosurgery, Yale University School of Medicine, New Haven, CT 06520, United States.

出版信息

Virology. 2015 Jan 15;475:1-14. doi: 10.1016/j.virol.2014.10.035. Epub 2014 Nov 21.

Abstract

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-α and to some extent with mycophenolic acid, chloroquine, and adenine 9-β-d-arabinofuranoside. To generate continuous IFN exposure, we made an adeno-associated virus vector expressing murine IFN; AAV-mIFN-β protected mouse brain cells from VSV, as did a combination of IFN, ribavirin and chloroquine. Intracranial AAV-mIFN-β protected the brain against VSV-CT9-M51. In SCID mice bearing human glioblastoma, AAV-mIFN-β moderately enhanced survival. VSV-CT9-M51 doubled median survival when administered after AAV-mIFN-β; 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.

摘要

水泡性口炎病毒(VSV)作为一种疫苗载体和溶瘤病毒显示出应用前景。然而,关于VSV神经毒性的报道仍然令人担忧。我们使用小鼠和人类脑培养物以及体内小鼠模型,比较了12种抗病毒化合物对VSV-CT9-M51和VSV-rp30感染的控制作用。利巴韦林和IFN-α对病毒复制、细胞毒性和感染性的抑制作用最强,霉酚酸、氯喹和腺嘌呤9-β-D-阿拉伯呋喃糖苷在一定程度上也有抑制作用。为了实现持续的IFN暴露,我们构建了一种表达小鼠IFN的腺相关病毒载体;AAV-mIFN-β保护小鼠脑细胞免受VSV感染,IFN、利巴韦林和氯喹的组合也有同样效果。颅内注射AAV-mIFN-β可保护大脑免受VSV-CT9-M51感染。在携带人胶质母细胞瘤的SCID小鼠中,AAV-mIFN-β适度延长了生存期。在AAV-mIFN-β给药后再给予VSV-CT9-M51,可使中位生存期延长一倍;一些存活的小鼠显示肿瘤完全被破坏。总之,这些数据表明AAV-IFN或IFN与利巴韦林和氯喹的组合为针对大脑中VSV的抗病毒治疗提供了最佳组合。

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