首页> 外文期刊>Journal of neurovirology >Neurovirulent factor ICP34.5 uniquely expressed in the herpes simplex virus type 1 Delta gamma 1 34.5 mutant 1716.
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Neurovirulent factor ICP34.5 uniquely expressed in the herpes simplex virus type 1 Delta gamma 1 34.5 mutant 1716.

机译:神经毒力因子ICP34.5在1型单纯疱疹病毒Deltaγ1 34.5突变体1716中唯一表达。

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The herpes simplex virus type 1 (HSV-1) diploid gene gamma(1)34.5 encodes a neurovirulent factor, infected cell protein 34.5 (ICP34.5). The promoter to gamma(1)34.5 is located within the HSV-1 genome where there are repeated sequences. This region of the genome also contains important overlapping transcripts involved with the virus's ability to establish lytic and latent infections and reactivation. These transcripts include the latency-associated transcripts and regulator proteins ICP0 and ICP4. This study aimed to separate ICP34.5 from these overlapping transcripts and test if its expression from a single gene could restore wild-type HSV-1 strain 17+ virulence. To address these aims, different recombinant viruses were constructed using the Delta gamma(1)34.5 mutant 1716. Immunoblots probed with different ICP34.5 antisera demonstrated that one of the newly generated recombinant viruses, 1622, overexpresses ICP34.5 relative to a panel of wild-type viruses. Interestingly, the overexpression of ICP34.5 does not yield a more virulent virus. The onset of ICP34.5 expression from 1622-infected cells in vitro matched that of 17+, and its expression restored the function of maintaining protein synthesis in human neuroblastoma cells. Replication of 1622, however, was only partially restored to 17+ levels in vivo. Additionally, plaque morphology from 1622-infected cells indicates there is an additional defect. The authors report that the mutant virus 1622 can express ICP34.5 from a single gamma(1)34.5 gene and restore most (but not all) wild-type function. These findings are discussed with respect to the use of the gamma(1)34.5 deleted mutant, 1716, in oncolytic viral vector therapies and future studies for ICP34.5.
机译:单纯疱疹病毒1型(HSV-1)二倍体基因gamma(1)34.5编码一种神经毒性因子,感染的细胞蛋白34.5(ICP34.5)。 γ(1)34.5的启动子位于HSV-1基因组中,那里有重复的序列。基因组的这一区域还包含重要的重叠转录本,与病毒建立裂解性和潜伏性感染以及再激活的能力有关。这些转录本包括与潜伏期相关的转录本和调节蛋白ICP0和ICP4。这项研究旨在从这些重叠的转录本中分离出ICP34.5,并测试其从单个基因中表达是否可以恢复野生型HSV-1毒株17+的毒力。为实现这些目标,使用Delta gamma(1)34.5突变体1716构建了不同的重组病毒。用不同ICP34.5抗血清探测的免疫印迹表明,一种新产生的重组病毒1622相对于一组ICP34.5过表达ICP34.5。野生型病毒。有趣的是,ICP34.5的过表达不会产生更具毒性的病毒。在体外,从1622年感染的细胞中ICP34.5的表达开始与17+相一致,并且其表达恢复了维持人类神经母细胞瘤细胞中蛋白质合成的功能。但是,体内的1622复制仅部分恢复到17+水平。此外,来自1622个感染细胞的噬菌斑形态表明存在其他缺陷。作者报告说,突变病毒1622可以从单个gamma(1)34.5基因表达ICP34.5,并且可以恢复大多数(但不是全部)野生型功能。这些发现是关于溶瘤病毒载体治疗和ICP34.5未来研究中使用gamma(1)34.5缺失突变体1716进行讨论的。

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