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Smad复合体与三联体DNA结合位点的相互作用。

Interaction of Smad complexes with tripartite DNA-binding sites.

作者信息

Johnson K, Kirkpatrick H, Comer A, Hoffmann F M, Laughon A

机构信息

Laboratory of Genetics, University of Wisconsin-Madison, Madison, Wisconsin 53706, USA.

出版信息

J Biol Chem. 1999 Jul 16;274(29):20709-16. doi: 10.1074/jbc.274.29.20709.

Abstract

The Smad family of transcription factors function as effectors of transforming growth factor-beta signaling pathways. Smads form heteromultimers capable of contacting DNA through the amino-terminal MH1 domain. The MH1 domains of Smad3 and Smad4 have been shown to bind to the sequence 5'-GTCT-3'. Here we show that Smad3 and Smad4 complexes can contact three abutting GTCT sequences and that arrays of such sites elevate reporter expression relative to arrays of binding sites containing only two GTCTs. Smad3/4 complexes bound synergistically to probes containing two of the four possible arrangements of three GTCT sequences and showed a correlated ability to synergistically activate transcription through these sites. Purified Smad3 and Smad4 were both able to contact three abutting GTCT sequences and reporter experiments indicated that either protein could mediate contact with all three GTCTs. In contrast, the Smad4 MH1 domain was essential for reporter activation in combination with Smad1. Together, these results show that Smad complexes are flexible in their ability to interact with abutting GTCT triplets. In contrast, Smads have high affinity for only one orientation of abutting GTCT pairs. Functional Smad-binding sites within several native response elements contain degenerate GTCT triplets, suggesting that trimeric Smad-DNA interaction may be relevant in vivo.

摘要

转录因子的Smad家族作为转化生长因子-β信号通路的效应器发挥作用。Smads形成能够通过氨基末端MH1结构域与DNA接触的异源多聚体。已证明Smad3和Smad4的MH1结构域与序列5'-GTCT-3'结合。在此我们表明,Smad3和Smad4复合物能够与三个相邻的GTCT序列接触,并且相对于仅包含两个GTCT的结合位点阵列,这些位点的阵列可提高报告基因的表达。Smad3/4复合物与包含三个GTCT序列的四种可能排列中的两种的探针协同结合,并显示出通过这些位点协同激活转录的相关能力。纯化的Smad3和Smad4都能够与三个相邻的GTCT序列接触,报告基因实验表明,任何一种蛋白质都可以介导与所有三个GTCT的接触。相比之下,Smad4的MH1结构域对于与Smad1结合时的报告基因激活至关重要。总之,这些结果表明,Smad复合物与相邻GTCT三联体相互作用的能力具有灵活性。相比之下,Smads对相邻GTCT对的仅一种方向具有高亲和力。几个天然反应元件内的功能性Smad结合位点包含简并的GTCT三联体,这表明三聚体Smad-DNA相互作用在体内可能是相关的。

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