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首页> 外文期刊>Journal of Molecular Biology >Molecular basis for bre5 cofactor recognition by the ubp3 deubiquitylating enzyme
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Molecular basis for bre5 cofactor recognition by the ubp3 deubiquitylating enzyme

机译:ubp3去泛素化酶识别bre5辅因子的分子基础

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Yeast Ubp3 and its co-factor Bre5 form a deubiquitylation complex to regulate protein transport between the endoplasmic reticulum and Golgi compartments of the cell. A novel N-terminal domain of the Ubp3 catalytic subunit forms a complex with the NTF2-like domain of the Bre5 regulatory subunit. Here, we report the X-ray crystal structure of an Ubp3-Bre5 complex and show that it forms a symmetric hetero-tetrameric complex in, which the Bre5 NTF2-like domain dimer interacts with two L-shaped beta-strand-turn-alpha-helix motifs of Ubp3. The Ubp3 N-terminal domain binds within a hydrophobic cavity on the surface of the Bre5 NTF2-like domain subunit with conserved residues within both proteins interacting predominantly through antiparallel beta-sheet hydrogen bonds and van der Waals contacts. Structure-based mutagenesis and functional studies confirm the significance of the observed interactions for Ubp3-Bre5 association in vitro and Ubp3 function in vivo. Comparison of the structure to other protein complexes with NTF2-like domains shows that the Ubp3-Bre5 interface is novel. Together, these studies provide new insights into Ubp3 recognition by Bre5 and into protein recognition by NTF2-like domains. (c) 2007 Elsevier Inc. All rights reserved.
机译:酵母Ubp3及其辅因子Bre5形成去泛素化复合物,以调节蛋白质在内质网和高尔基体之间的蛋白运输。 Ubp3催化亚基的新的N末端域与Bre5调节亚基的NTF2样域形成复合物。在这里,我们报告了Ubp3-Bre5复合物的X射线晶体结构,并表明它形成了对称的异四聚体复合物,其中Bre5 NTF2样结构域二聚体与两个L形β-链-转角-α相互作用-bp的Ubp3螺旋基序。 Ubp3 N末端结构域与Bre5 NTF2类结构域亚基表面的疏水腔内结合,两个蛋白质中的保守残基主要通过反平行的β-折叠氢键和范德华接触相互作用。基于结构的诱变和功能研究证实了观察到的相互作用对于体外Ubp3-Bre5关联和体内Ubp3功能的重要性。与具有NTF2类结构域的其他蛋白质复合物的结构比较表明,Ubp3-Bre5接口是新颖的。总之,这些研究为Bre5对Ubp3的识别以及NTF2样结构域对蛋白质的识别提供了新的见解。 (c)2007 Elsevier Inc.保留所有权利。

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