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首页> 外文期刊>Journal of Virology >Identification and characterization of a major early cytomegalovirus DNA-binding protein.
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Identification and characterization of a major early cytomegalovirus DNA-binding protein.

机译:主要早期细胞瘤病毒DNA结合蛋白的鉴定与表征。

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摘要

We characterized a DNA-binding protein with an approximate molecular weight of 129,000 (DB129) which is present in the nuclei of cytomegalovirus- (strain Colburn) infected cells, but not in virus particles. Results of two types of experiments demonstrated that DB129 is a member of the early class of herpesviral proteins. First, time course pulse-labeling experiments showed that its synthesis begins after that of the immediate-early protein IE94, but prior to the appearance of late viral proteins, and was reduced at late times. Second, in the presence of inhibitors of viral DNA replication, DB129 continued to be made and accumulated to elevated levels. A second set of experiments showed that DB129 bound to single-stranded DNA in vitro and was eluted by a NaCl gradient in two peaks, one at about 0.2 M and the second at about 0.6 M. A similar pattern of release was observed when infected-cell nuclei were serially extracted with increasing NaCl concentrations. In addition, treatment of nuclei with DNase I selectively released DB129, along with a small but significant fraction of another DNA-binding protein, DB51. These results suggest that DB129 is associated with DNA in vivo and that it interacts directly with single-stranded DNA. It was also shown that cells infected with human cytomegalovirus (strain Towne) contain a slightly larger counterpart to DB129, which was designated DB140. Similarities between these proteins and the major DNA-binding protein of herpes simplex virus are discussed.
机译:我们的表征具有近似分子量为129,000(DB129)的DNA结合蛋白,其存在于细胞核病毒 - (菌株COLBurn)感染细胞的细胞核中,但不在病毒颗粒中。两种实验的结果证明DB129是早期疱疹病毒蛋白的成员。首先,时间过程脉冲标记实验表明,其合成之后在立即早期蛋白IE94之后开始,但在晚期病毒蛋白外出现之前,在晚期降低。其次,在存在病毒DNA复制的抑制剂存在下,DB129继续进行并累积至升高的水平。第二组实验表明,DB129在体外结合到单链DNA,并在两个峰的NaCl梯度洗脱,在约0.2μm,秒为约0.6米。当感染时观察到类似的释放模式随着NaCl浓度的增加,串联提取细胞核。此外,用DNA酶治疗核,IS选择性地释放DB129,以及另一个DNA结合蛋白DB51的小但显着的部分。这些结果表明DB129与体内DNA相关,并且它与单链DNA直接相互作用。还显示出用人巨细胞病毒(菌株Towne)感染的细胞含有略微较大的对应于DB129,其被指定为DB140。讨论了这些蛋白质与单纯疱疹病毒的主要DNA结合蛋白质之间的相似性。

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