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Ultrastructural Analysis of ICP34.5− Herpes Simplex Virus 1 Replication in Mouse Brain Cells In Vivo

机译:ICP34.5−单纯疱疹病毒1在小鼠脑细胞体内复制的超微结构分析

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摘要

Replication-competent forms of herpes simplex virus 1 (HSV-1) defective in the viral neurovirulence factor infected cell protein 34.5 (ICP34.5) are under investigation for use in the therapeutic treatment of cancer. In mouse models, intratumoral injection of ICP34.5-defective oncolytic HSVs (oHSVs) has resulted in the infection and lysis of tumor cells, an associated decrease in tumor size, and increased survival times. The ability of these oHSVs to infect and lyse cells is frequently characterized as exclusive to or selective for tumor cells. However, the extent to which ICP34.5-deficient HSV-1 replicates in and may be neurotoxic to normal brain cell types in vivo is poorly understood. Here we report that HSV-1 defective in ICP34.5 expression is capable of establishing a productive infection in at least one normal mouse brain cell type. We show that γ34.5 deletion viruses replicate productively in and induce cellular damage in infected ependymal cells. Further evaluation of the effects of oHSVs on normal brain cells in animal models is needed to enhance our understanding of the risks associated with the use of current and future oHSVs in the brains of clinical trial subjects and to provide information that can be used to create improved oHSVs for future use.
机译:目前正在研究在病毒神经毒力因子感染的细胞蛋白34.5(ICP34.5)中有缺陷的具有复制能力的单纯疱疹病毒1(HSV-1)的形式,以用于癌症的治疗。在小鼠模型中,瘤内注射ICP34.5缺陷的溶瘤HSV(oHSV)已导致肿瘤细胞的感染和裂解,伴随着肿瘤尺寸的减小和存活时间的延长。这些oHSV感染和裂解细胞的能力通常被表征为对肿瘤细胞具有排他性或选择性。但是,对ICP34.5缺失的HSV-1在体内复制的程度以及对体内正常脑细胞类型的神经毒性的了解甚少。在这里我们报告ICP34.5表达缺陷的HSV-1能够在至少一种正常小鼠脑细胞类型中建立生产性感染。我们表明,γ34.5缺失病毒在感染的室管膜细胞中高效复制并诱导细胞损伤。需要进一步评估oHSV对动物模型中正常脑细胞的作用,以加深我们对与在临床试验对象的大脑中使用当前和将来的oHSV相关的风险的了解,并提供可用于创造改善的信息oHSV供将来使用。

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