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利用DNA的羟基自由基切割和甲基化干扰研究同源结构域-亮氨酸拉链/DNA复合物的结构

Structure of homeodomain-leucine zipper/DNA complexes studied using hydroxyl radical cleavage of DNA and methylation interference.

作者信息

Tron Adriana E, Comelli Raúl N, Gonzalez Daniel H

机构信息

Facultad de Bioquímica y Ciencias Biológicas, Universidad Nacional del Litoral, CC 242 Paraje El Pozo, 3000 Santa Fe, Argentina.

出版信息

Biochemistry. 2005 Dec 27;44(51):16796-803. doi: 10.1021/bi0513150.

Abstract

Homeodomain-leucine zipper (HD-Zip) proteins, unlike most homeodomain proteins, bind a pseudopalindromic DNA sequence as dimers. We have investigated the structure of the DNA complexes formed by two HD-Zip proteins with different nucleotide preferences at the central position of the binding site using footprinting and interference methods. The results indicate that the respective complexes are not symmetric, with the strand bearing a central purine (top strand) showing higher protection around the central region and the bottom strand protected toward the 3' end. Binding to a sequence with a nonpreferred central base pair produces a decrease in protection in either the top or the bottom strand, depending upon the protein. Modeling studies derived from the complex formed by the monomeric Antennapedia homeodomain with DNA indicate that in the HD-Zip/DNA complex the recognition helix of one of the monomers is displaced within the major groove respective to the other one. This monomer seems to lose contacts with a part of the recognition sequence upon binding to the nonpreferred site. The results show that the structure of the complex formed by HD-Zip proteins with DNA is dependent upon both protein intrinsic characteristics and the nucleotides present at the central position of the recognition sequence.

摘要

与大多数同源结构域蛋白不同,同源结构域-亮氨酸拉链(HD-Zip)蛋白以二聚体形式结合假回文DNA序列。我们使用足迹法和干涉法研究了两种在结合位点中心位置具有不同核苷酸偏好的HD-Zip蛋白所形成的DNA复合物的结构。结果表明,各自的复合物不对称,带有中心嘌呤的链(顶链)在中心区域周围显示出更高的保护,而底链在3'端受到保护。与具有非优选中心碱基对的序列结合会导致顶链或底链的保护降低,这取决于蛋白质。从单体触角足同源结构域与DNA形成的复合物进行的建模研究表明,在HD-Zip/DNA复合物中,其中一个单体的识别螺旋相对于另一个单体在大沟内发生位移。该单体在与非优选位点结合时似乎失去了与部分识别序列的接触。结果表明,HD-Zip蛋白与DNA形成的复合物的结构取决于蛋白质的固有特性以及识别序列中心位置存在的核苷酸。

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