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Expression of the herpes simplex virus type 1 latency-associated transcripts does not influence latency establishment of virus mutants deficient for neuronal replication

机译:单纯疱疹病毒1型潜伏期相关转录本的表达不影响缺乏神经元复制的病毒突变体的潜伏期

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摘要

Herpes simplex virus type 1 establishes latency within neurons of the trigeminal ganglion. During latency, viral gene expression is largely restricted to the latency-associated transcripts (LATs), which, whilst not essential for any aspect of latency, function to suppress lytic gene expression and enhance the survival of virus-infected neurons. The latent cell population comprises primary-order neurons infected directly from peripheral tissues and cells infected following further virus spread within the ganglion. In order to assess the role of LAT expression on latency establishment within first-order neurons, we infected ROSA26R reporter mice with Cre recombinase-expressing recombinant viruses harbouring deletion of the thymidine kinase lytic gene and/or the core LAT promoter. We found that LAT expression did not impact on latency establishment in viruses unable to replicate in neurons, and under these conditions, it was not required for the survival of neurons between 3 and 31 days post-infection.
机译:1型单纯疱疹病毒在三叉神经节的神经元内建立潜伏期。在潜伏期中,病毒基因表达在很大程度上受潜伏期相关转录本(LATs)的限制,尽管对潜伏期的任何方面都不是必需的,但其功能是抑制裂解基因表达并增强病毒感染的神经元的存活。潜伏细胞群包括直接从周围组织感染的初级神经元和在神经节内进一步传播病毒后感染的细胞。为了评估LAT表达对一级神经元内潜伏期建立的作用,我们用表达Cre重组酶的重组病毒感染了ROSA26R报告基因小鼠,所述重组病毒带有胸苷激酶裂解基因和/或核心LAT启动子的缺失。我们发现,在无法在神经元中复制的病毒中,LAT表达不会影响潜伏期的建立,在这种情况下,感染后3到31天之间,神经元的存活并不需要它。

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