p53的序列特异性核心结构域与非特异性C末端DNA结合结构域之间的相互干扰:对调控的影响
Reciprocal interference between the sequence-specific core and nonspecific C-terminal DNA binding domains of p53: implications for regulation.
作者信息
Anderson M E, Woelker B, Reed M, Wang P, Tegtmeyer P
机构信息
Department of Molecular Genetics and Microbiology, State University of New York, Stony Brook 11794-5222, USA.
出版信息
Mol Cell Biol. 1997 Nov;17(11):6255-64. doi: 10.1128/MCB.17.11.6255.
Abstract
The tumor suppressor p53 has two DNA binding domains: a central sequence-specific domain and a C-terminal sequence-independent domain. Here, we show that binding of large but not small DNAs by the C terminus of p53 negatively regulates sequence-specific DNA binding by the central domain. Four previously described mechanisms for activation of specific DNA binding operate by blocking negative regulation. Deletion of the C terminus of p53 activates specific DNA binding only in the presence of large DNA. Three activator molecules (a small nucleic acid, a monoclonal antibody against the p53 C terminus, and a C-terminal peptide of p53) stimulate sequence-specific DNA binding only in the presence of both large DNA and p53 with an intact C terminus. Our findings argue that interactions of the C terminus of p53 with genomic DNA in vivo would prevent p53 binding to specific promoters and that cellular mechanisms to block C-terminal DNA binding would be required.
摘要
肿瘤抑制因子p53有两个DNA结合结构域:一个中央序列特异性结构域和一个C端序列非依赖性结构域。在此,我们表明,p53的C端与大DNA而非小DNA的结合会负向调节中央结构域的序列特异性DNA结合。之前描述的四种激活特异性DNA结合的机制是通过阻断负调节来起作用的。删除p53的C端仅在存在大DNA的情况下才会激活特异性DNA结合。三种激活分子(一种小核酸、一种抗p53 C端的单克隆抗体和p53的C端肽)仅在同时存在大DNA和具有完整C端的p53时才会刺激序列特异性DNA结合。我们的研究结果表明,p53的C端在体内与基因组DNA的相互作用会阻止p53与特定启动子结合,并且需要细胞机制来阻断C端与DNA的结合。
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