首页> 美国卫生研究院文献>Nucleic Acids Research >The DNA binding domains of the varicella-zoster virus gene 62 and herpes simplex virus type 1 ICP4 transactivator proteins heterodimerize and bind to DNA.
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The DNA binding domains of the varicella-zoster virus gene 62 and herpes simplex virus type 1 ICP4 transactivator proteins heterodimerize and bind to DNA.

机译:水痘带状疱疹病毒基因62和1型单纯疱疹病毒ICP4反式激活蛋白的DNA结合结构域异源二聚体并与DNA结合。

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摘要

The product of varicella-zoster virus gene 62 (VZV 140k) is the functional counterpart of the major transcriptional regulatory protein of herpes simplex virus type 1 (HSV-1), ICP4. We have found that the purified bacterially expressed DNA binding domain of VZV 140k (residues 417-647) is a stable dimer in solution. As demonstrated by the appearance of a novel protein--DNA complex of intermediate mobility in gel retardation assays, following in vitro co-translation of a pair of differently sized VZV 140k DNA binding domain peptides, the 140k DNA binding domain peptide binds to DNA as a dimer. In addition, the DNA binding domain peptide of HSV-1 ICP4 readily heterodimerizes with the VZV 140k peptide on co-translation, indicating that HSV-1 ICP4 and VZV 140k possess very similar dimerization interfaces. It appears that only one fully wild type subunit of the dimer is sufficient to mediate sequence specific DNA recognition in certain circumstances. Co-immunoprecipitation analysis of mutant DNA binding domain peptides, co-translated with an epitope-tagged ICP4 DNA binding domain, shows that the sequence requirements for dimerization are lower than those necessary for DNA binding.
机译:水痘带状疱疹病毒基因62(VZV 140k)的产物与单纯疱疹病毒1型(HSV-1)ICP4的主要转录调节蛋白功能相同。我们已经发现,纯化的细菌表达的VZV 140k的DNA结合结构域(残基417-647)在溶液中是稳定的二聚体。如在凝胶阻滞测定法中出现的一种新型蛋白-中等迁移率的DNA复合物的出现所证明的,在一对不同大小的VZV 140k DNA结合结构域肽在体外共翻译后,140k DNA结合结构域肽以如下方式结合到DNA二聚体。此外,HSV-1 ICP4的DNA结合结构域肽在共翻译时很容易与VZV 140k肽异二聚,表明HSV-1 ICP4和VZV 140k具有非常相似的二聚化界面。在某些情况下,似乎只有一个二聚体的完全野生型亚基足以介导序列特异性DNA识别。与表位标记的ICP4 DNA结合结构域共翻译的突变DNA结合结构域肽的共免疫沉淀分析表明,二聚化的序列要求低于DNA结合所需的序列要求。

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