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八聚体结合蛋白Oct-2可抑制病毒体蛋白Vmw65对单纯疱疹病毒立即早期基因的反式激活作用。

The octamer binding protein Oct-2 inhibits transactivation of the herpes simplex virus immediate-early genes by the virion protein Vmw65.

作者信息

Lillycrop K A, Estridge J K, Latchman D S

机构信息

Division of Molecular Pathology, University College London Medical School, United Kingdom.

出版信息

Virology. 1993 Oct;196(2):888-91. doi: 10.1006/viro.1993.1552.

Abstract

Transactivation by a complex of the cellular transcription factor Oct-1 and the virion protein Vmw65 is necessary for the high-level activity of the HSV immediate-early promoters during lytic infection. We show that this trans-activation can be inhibited by two forms of the Oct-2 transcription factor which are expressed at high levels in neuronal cells as well as by the isolated DNA binding, POU domain of Oct-2. The inhibition of Oct-1-Vmw65 DNA binding by these neuronal forms of Oct-2 is likely to play a critical role in the nonpermissivity of neuronal cells for the HSV lytic cycle and therefore in the establishment of latent infections.

摘要

在裂解感染期间,细胞转录因子Oct-1和病毒体蛋白Vmw65的复合物进行反式激活对于单纯疱疹病毒(HSV)立即早期启动子的高水平活性是必需的。我们发现,这种反式激活可被在神经元细胞中高水平表达的两种Oct-2转录因子形式以及Oct-2的分离的DNA结合POU结构域所抑制。这些神经元形式的Oct-2对Oct-1-Vmw65 DNA结合的抑制作用可能在神经元细胞对HSV裂解周期的非允许性中起关键作用,因此在潜伏感染的建立中也起关键作用。

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