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Multiple functions of the nonconserved N-terminal domain of yeast TATA-binding protein.

机译:酵母TATA结合蛋白的非保守N末端结构域的多功能。

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摘要

The TATA-binding protein (TBP) is composed of a highly conserved core domain sufficient for TATA-element binding and preinitiation complex formation as well as a highly divergent N-terminal region that is dispensable for yeast cell viability. In vitro, removal of the N-terminal region domain enhances TBP-TATA association and TBP dimerization. Here, we examine the effects of truncation of the N-terminal region in the context of yeast TBP mutants with specific defects in DNA binding and in interactions with various proteins. For a subset of mutations that disrupt DNA binding and the response to transcriptional activators, removal of the N-terminal domain rescues their transcriptional defects. By contrast, deletion of the N-terminal region is lethal in combination with mutations on a limited surface of TBP. Although this surface is important for interactions with TFIIA and Brf1, TBP interactions with these two factors do not appear to be responsible for this dependence on the N-terminal region. Our results suggest that the N-terminal region of TBP has at least two distinct functions in vivo. It inhibits the interaction of TBP with TATA elements, and it acts positively in combination with a specific region of the TBP core domain that presumably interacts with another protein(s).
机译:TATA结合蛋白(TBP)由足以保存TATA元素结合和预起始复合物形成的高度保守的核心结构域,以及为酵母细胞生存能力所必需的高度分歧的N端区域组成。在体外,去除N末端区域结构域可增强TBP-TATA缔合和TBP二聚化。在这里,我们检查在酵母TBP突变体的背景下N末端区域被截断的影响,该突变体在DNA结合以及与各种蛋白质的相互作用中具有特定缺陷。对于破坏DNA结合和对转录激活因子反应的突变的子集,去除N末端结构域可挽救其转录缺陷。相反,结合TBP有限表面上的突变,N末端区域的缺失是致命的。尽管此表面对于与TFIIA和Brf1的相互作用很重要,但是与这两个因子的TBP相互作用似乎并不负责这种对N末端区域的依赖性。我们的结果表明,TBP的N端区域在体内至少具有两个不同的功能。它抑制TBP与TATA元素的相互作用,并且与TBP核心域的特定区域(可能与另一种蛋白质相互作用)结合而发挥积极作用。

著录项

  • 期刊名称 Genetics
  • 作者

    M Lee; K Struhl;

  • 作者单位
  • 年(卷),期 2001(158),1
  • 年度 2001
  • 页码 87–93
  • 总页数 7
  • 原文格式 PDF
  • 正文语种
  • 中图分类 遗传学;
  • 关键词

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