首页> 美国卫生研究院文献>Acta Crystallographica Section F: Structural Biology and Crystallization Communications >Crystallization and preliminary X-ray crystallographic analysis of the N domain of p97/VCP in complex with the UBX domain of FAF1
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Crystallization and preliminary X-ray crystallographic analysis of the N domain of p97/VCP in complex with the UBX domain of FAF1

机译:与FAF1的UBX结构域复合的p97 / VCP N结构域的结晶和初步X射线晶体学分析

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摘要

p97/VCP is a multifunctional AAA+-family ATPase that is involved in diverse cellular processes. p97/VCP directly interacts with various adaptors for activity in different biochemical contexts. Among these adaptors are p47 and Fas-associated factor 1 (FAF1), which contain a common UBX domain through which they bind to the N domain of p97/VCP. In the ubiquitin–proteasome pathway, p97/VCP acts as a chaperone that presents client proteins to the proteasome for degradation, while FAF1 modulates the process by interacting with ubiquitinated client proteins and also with p97/VCP. In an effort to elucidate the structural details of the interaction between p97/VCP and FAF1, the p97/VCP N domain was crystallized in complex with the FAF1 UBX domain. X-ray data were collected to 2.60 Å resolution and the crystals belonged to space group C2221, with unit-cell parameters a = 58.24, b = 72.81, c = 132.93 Å. The Matthews coefficient and solvent content were estimated to be 2.39 Å3 Da−1 and 48.4%, respectively, assuming that the asymmetric unit contained p97/VCP N domain and FAF1 molecules in a 1:1 ratio, which was subsequently confirmed by molecular-replacement calculations.
机译:p97 / VCP是一种多功能的AAA + 家族ATPase,参与多种细胞过程。 p97 / VCP直接与各种衔接子相互作用,以在不同的生化环境中发挥活性。这些衔接子中有p47和Fas相关因子1(FAF1),它们包含一个公用UBX域,通过它们它们与p97 / VCP的N域结合。在泛素-蛋白酶体途径中,p97 / VCP充当伴侣,将客体蛋白提供给蛋白酶体进行降解,而FAF1通过与泛素化的客体蛋白以及p97 / VCP相互作用来调节过程。为了阐明p97 / VCP和FAF1之间相互作用的结构细节,使p97 / VCP N结构域与FAF1 UBX结构域复合结晶。收集到的X射线数据分辨率为2.60Å,晶体属于C2221空间群,单位晶胞参数a = 58.24,b = 72.81,c = 132.93。假设不对称单元包含p97 / VCP N域和FAF1分子,则马修斯系数和溶剂含量分别估计为2.39Å 3 Da -1 和48.4%。比例为1:1,随后通过分子取代计算得到了证实。

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