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巴赫1(Bach1)BTB结构域的晶体结构及其对同源二聚化的调控

Crystal structure of the Bach1 BTB domain and its regulation of homodimerization.

作者信息

Ito Nobutoshi, Watanabe-Matsui Miki, Igarashi Kazuhiko, Murayama Kazutaka

机构信息

Biomedical Engineering Research Organization, Tohoku University, Aoba-ku, Sendai, Japan.

出版信息

Genes Cells. 2009 Feb;14(2):167-78. doi: 10.1111/j.1365-2443.2008.01259.x. Epub 2008 Jan 12.

Abstract

The BTB/POZ domain is known as a protein-protein interaction motif that mediates homodimer and higher order self-associations. Proteins containing the BTB domain exist throughout eukaryotes; however, there is little information about the mechanism that determines the oligomeric state of the BTB domain. To address this question, we have determined the X-ray structure of the mouse Bach1 BTB domain. The present structure is similar to the previously determined BTB domain folds, including the human Bach1 BTB domain; however, distinct structural features are present, such as a novel homodimer interaction surface. The homodimer formation was found to involve a novel hydrogen bond network and interactions between hydrophobic surfaces of the kinked N-terminus (N-hook) and the partner's C-terminal residues. The deletion of the N-hook resulted in the conversion of the homodimer into a monomer in solution, indicating that the N-hook promotes the homodimerization of the mBach1 BTB domain. We have also found that the BTB domain of Bach2, a protein highly related to Bach1, is present as a monomer due to a short peptide insertion at the N-hook. These results represent the first example of the key modulatory element of BTB domain homodimerization.

摘要

BTB/POZ结构域是一种已知的蛋白质-蛋白质相互作用基序,介导同型二聚体和更高阶的自缔合。含有BTB结构域的蛋白质存在于整个真核生物中;然而,关于决定BTB结构域寡聚状态的机制的信息却很少。为了解决这个问题,我们确定了小鼠Bach1 BTB结构域的X射线结构。目前的结构与先前确定的BTB结构域折叠相似,包括人Bach1 BTB结构域;然而,存在独特的结构特征,例如一个新的同型二聚体相互作用表面。发现同型二聚体的形成涉及一个新的氢键网络以及扭结的N端(N钩)疏水表面与伙伴C端残基之间的相互作用。N钩的缺失导致同型二聚体在溶液中转变为单体,表明N钩促进了mBach1 BTB结构域的同型二聚化。我们还发现,与Bach1高度相关的蛋白质Bach2的BTB结构域由于在N钩处有一个短肽插入而以单体形式存在。这些结果代表了BTB结构域同型二聚化关键调节元件的首个实例。

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