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配对的类同源结构域蛋白介导的位点特异性异源二聚化作用可调节选择性转录反应。

Site-specific heterodimerization by paired class homeodomain proteins mediates selective transcriptional responses.

作者信息

Tucker S C, Wisdom R

机构信息

Department of Biochemistry, Vanderbilt University, Nashville, Tennessee 37232, USA.

出版信息

J Biol Chem. 1999 Nov 5;274(45):32325-32. doi: 10.1074/jbc.274.45.32325.

Abstract

Alx4 is a paired class homeodomain protein involved in defining anterior/posterior polarity in the developing limb bud. The paired class of homeodomain proteins cooperatively bind palindromic DNA elements as homodimers or as heterodimers with other paired homeodomain proteins. Previous characterization demonstrates that the strength of the cooperativity as well as the preference for targets is dictated largely by the identity of amino acid 50 of the homeodomain. Here we compare and contrast the DNA binding properties of a glutamine 50 paired homeodomain protein, Alx4, and a lysine 50 paired homeodomain protein, Goosecoid. We demonstrate that Alx4 homodimers, Gsc homodimers, and Alx4/Gsc heterodimers each have distinct DNA binding properties, and each can discriminate between highly related palindromic elements. Using reporter gene assays, we show that Alx4 activates transcription in a site-specific manner, and that Gsc is capable of antagonizing Alx4-mediated activation only from promoter elements that support heterodimer formation. These data demonstrate that paired homeodomain proteins with different DNA binding properties are able to form heterodimeric complexes with unique DNA binding and transcriptional activities. Thus, heterodimerization regulates the DNA binding specificity of these transcription factors and may partially explain how paired homeodomain proteins direct specific developmental functions.

摘要

Alx4是一种配对型同源结构域蛋白,参与确定发育中的肢芽的前后极性。同源结构域蛋白的配对型以同二聚体形式或与其他配对型同源结构域蛋白形成异二聚体的形式协同结合回文DNA元件。先前的特征表明,协同作用的强度以及对靶标的偏好很大程度上由同源结构域的第50位氨基酸的特性决定。在这里,我们比较并对比了第50位氨基酸为谷氨酰胺的配对型同源结构域蛋白Alx4和第50位氨基酸为赖氨酸的配对型同源结构域蛋白Goosecoid的DNA结合特性。我们证明,Alx4同二聚体、Gsc同二聚体以及Alx4/Gsc异二聚体各自具有独特的DNA结合特性,并且它们都能够区分高度相关的回文元件。使用报告基因检测,我们表明Alx4以位点特异性方式激活转录,并且Gsc仅能够从支持异二聚体形成的启动子元件拮抗Alx4介导的激活。这些数据表明,具有不同DNA结合特性的配对型同源结构域蛋白能够形成具有独特DNA结合和转录活性的异二聚体复合物。因此,异二聚化调节这些转录因子的DNA结合特异性,并且可能部分解释了配对型同源结构域蛋白如何指导特定的发育功能。

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