首页> 美国卫生研究院文献>Journal of Virology >A novel sequence-specific DNA-binding protein LCP-1 interacts with single-stranded DNA and differentially regulates early gene expression of the human neurotropic JC virus.
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A novel sequence-specific DNA-binding protein LCP-1 interacts with single-stranded DNA and differentially regulates early gene expression of the human neurotropic JC virus.

机译:一种新型的序列特异性DNA结合蛋白LCP-1与单链DNA相互作用并差异性调节人类嗜神经性JC病毒的早期基因表达。

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摘要

We have identified a novel brain-derived single-stranded-DNA-binding protein that interacts with a region of the human neurotropic JC virus enhancer designated the lytic control element (LCE). This nuclear factor, LCP-1 (for lytic control element-binding protein 1), specifically recognizes the LCE, as determined by gel retardation assays. Alkylation interference showed that specific nucleotides within the LCE were contacted by LCP-1. Subsequent experiments revealed that point mutations within the LCE differentially affected LCP-1 binding. UV cross-linking and competition analysis suggested that the LCP-1 DNA-protein complexes were 50 to 52 and 100 to 120 kDa in size. Promoter mutations that affected LCP-1 binding reduced early mRNA transcription during the early phase of the lytic cycle. However, upon DNA replication in the presence of JC virus T antigen, when early mRNA initiation shifts to new locations indicative of the late phase, the LCP-1 mutations had no effect. We suggest that the JC virus early transcription unit is differentially regulated by LCP-1 prior to but not after DNA replication, suggesting a novel mechanism by which DNA structure regulates eukaryotic gene expression.
机译:我们已经确定了一种新型的脑源性单链DNA结合蛋白,该蛋白与人类嗜神经性JC病毒增强子的区域相互作用,称为裂解控制元件(LCE)。该核因子LCP-1(用于裂解性控制元件结合蛋白1)特异性识别LCE,通过凝胶阻滞测定法确定。烷基化干扰显示LCP-1接触了LCE中的特定核苷酸。随后的实验表明,LCE中的点突变差异地影响了LCP-1的结合。紫外线交联和竞争分析表明,LCP-1 DNA-蛋白质复合物的大小为50至52和100至120 kDa。影响LCP-1结合的启动子突变降低了裂解周期早期的早期mRNA转录。但是,在存在JC病毒T抗原的情况下进行DNA复制后,当早期的mRNA起始转移到指示晚期的新位置时,LCP-1突变将无效。我们建议JC病毒早期转录单位是由LCP-1在DNA复制之前而不是在DNA复制之后进行差异调节的,这表明DNA结构调节真核基因表达的新机制。

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