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首页> 外文期刊>Virology >Human papillomavirus 16 E2 stability and transcriptional activation is enhanced by E1 via a direct protein-protein interaction.
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Human papillomavirus 16 E2 stability and transcriptional activation is enhanced by E1 via a direct protein-protein interaction.

机译:人乳头瘤病毒16 E2的稳定性和转录激活通过直接的蛋白质-蛋白质相互作用被E1增强。

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Human papillomavirus 16 E1 and E2 interact with cellular factors to replicate the viral genome. E2 forms homodimers and binds to 12 bp palindromic sequences adjacent to the viral origin and recruits E1 to the origin. E1 forms a di-hexameric helicase complex that replicates the viral genome. This manuscript demonstrates that E1 stabilises the E2 protein, increasing the half life in both C33a and 293 T cells respectively. This stabilisation requires a direct protein--protein interaction. In addition, the E1 protein enhances E2 transcription function in a manner that suggests the E1 protein itself can contribute to transcriptional regulation not simply by E2 stabilisation but by direct stimulation of transcription. This activation of E2 transcription is again dependent upon an interaction with E1. Overall the results suggest that in the viral life cycle, co-expression of E1 with E2 can increase E2 stability and enhance E2 function.
机译:人乳头瘤病毒16 E1和E2与细胞因子相互作用,复制病毒基因组。 E2形成同型二聚体并与病毒起源附近的12 bp回文序列结合,并将E1募集到该起源。 E1形成复制病毒基因组的二六聚解旋酶复合物。该手稿表明,E1可以稳定E2蛋白,从而分别延长C33a和293 T细胞的半衰期。这种稳定作用需要直接的蛋白质-蛋白质相互作用。此外,E1蛋白以某种方式增强E2转录功能,表明E1蛋白本身不仅可以通过E2稳定,而且可以通过直接刺激转录来促进转录调控。 E2转录的这种激活再次取决于与E1的相互作用。总体而言,结果表明在病毒生命周期中,E1与E2的共表达可以增加E2的稳定性并增强E2的功能。

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