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人嗜T淋巴细胞病毒1型(HTLV-1)Tax蛋白具有不同但相互重叠的转录激活结构域和增强子特异性结构域。

HTLV-1 Tax has distinct but overlapping domains for transcriptional activation and for enhancer specificity.

作者信息

Fujii M, Tsuchiya H, Seiki M

机构信息

Department of Virology, Cancer Research Institute, Ishikawa, Japan.

出版信息

Oncogene. 1991 Dec;6(12):2349-52.

PMID:1766679
Abstract

Tax1 of human T-cell leukemia virus type 1 (HTLV-1) activates viral transcription dependent upon three 21-bp enhancer elements in the long terminal repeat. Difficulties in detecting any association of Tax1 with the viral enhancer have hampered elucidation of the molecular mechanisms of Tax1-mediated transcriptional activation. By constructing a fusion protein with the heterologous DNA-binding domain of yeast GAL4, Tax1 was shown to be a potent transcriptional activator dependent on the presence of GAL4-binding sites. Deletions of the Tax1 portion of the fusion protein revealed that almost the entire region of Tax1 (amino acids 2-337) is required for activation, and the activity correlated well with that of the viral enhancer. The GAL/Tax1 mutant lacking 41 residues of the C-terminus of Tax1, GAL/Tax1(2-312), was inactive for the viral enhancer, but activity was recovered by adding the heterologous activation domain of herpes simplex virus VP16. These results indicate that Tax1 has two distinct but overlapping functional domains for transcriptional activation and for enhancer specificity. Thus, Tax1 is thought to be a transcription factor acting in the enhancer complex rather than as a catalytic or allosteric modifier of pre-existing cellular transcription factors.

摘要

人类嗜T细胞病毒1型(HTLV-1)的Tax1蛋白可激活依赖于长末端重复序列中三个21碱基对增强子元件的病毒转录。检测Tax1与病毒增强子之间的任何关联存在困难,这阻碍了对Tax1介导的转录激活分子机制的阐明。通过构建与酵母GAL4异源DNA结合结构域的融合蛋白,Tax1被证明是一种依赖于GAL4结合位点存在的强效转录激活因子。对融合蛋白中Tax1部分的缺失分析表明,Tax1几乎整个区域(氨基酸2 - 337)对于激活都是必需的,并且其活性与病毒增强子的活性密切相关。缺少Tax1蛋白C末端41个残基的GAL/Tax1突变体GAL/Tax1(2 - 312)对病毒增强子无活性,但通过添加单纯疱疹病毒VP16的异源激活结构域可恢复其活性。这些结果表明,Tax1具有两个不同但重叠的功能结构域,分别用于转录激活和增强子特异性。因此,Tax1被认为是一种在增强子复合物中起作用的转录因子,而不是作为已存在的细胞转录因子的催化或变构修饰剂。

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