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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >The Roc‐COR tandem domain of leucine‐rich repeat kinase 2 forms dimers and exhibits conventional Ras‐like GTPase properties
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The Roc‐COR tandem domain of leucine‐rich repeat kinase 2 forms dimers and exhibits conventional Ras‐like GTPase properties

机译:富含亮氨酸的重复激酶2的ROC-COR串联结构域形成二聚体并表现出常规的RAS样GTP酶属性

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Abstract The Parkinson's disease ( PD )‐causative leucine‐rich repeat kinase 2 ( LRRK 2) belongs to the Roco family of G‐proteins comprising a Ras‐of‐complex (Roc) domain followed by a C‐terminal of Roc ( COR ) domain in tandem (called Roc‐ COR domain). Two prokaryotic Roc‐ COR domains have been characterized as ‘G proteins activated by guanine nucleotide‐dependent dimerization’ ( GAD s), which require dimerization for activation of their GTP ase activity and bind guanine nucleotides with relatively low affinities. Additionally, LRRK 2 Roc domain in isolation binds guanine nucleotides with relatively low affinities. As such, LRRK 2 GTP ase domain was predicted to be a GAD . Herein, we describe the design and high‐level expression of human LRRK 2 Roc‐ COR domain ( LRRK 2 Roc‐ COR ). Biochemical analyses of LRRK 2 Roc‐ COR reveal that it forms homodimers, with the C‐terminal portion of COR mediating its dimerization. Furthermore, it co‐purifies and binds Mg 2+ GTP / GDP at 1?:?1 stoichiometry, and it hydrolyzes GTP with K m ?and? k cat? of 22 nM and 4.70?×?10 ?4 ?min ?1 , ? respectively. Thus, even though LRRK 2 Roc‐ COR forms GAD ‐like homodimers, it exhibits conventional Ras‐like GTP ase properties, with high‐affinity binding of Mg 2+ ‐ GTP / GDP and low intrinsic catalytic activity. The PD ‐causative Y1699C mutation mapped to the COR domain was previously reported to reduce the GTP ase activity of full‐length LRRK 2. In contrast, this mutation induces no change in the GTP ase activity, and only slight perturbations in the secondary structure contents of LRRK 2 Roc‐ COR . As this mutation does not directly affect the GTP ase activity of the isolated Roc‐ COR tandem, it is possible that the effects of this mutation on full‐length LRRK 2 occur via other functional domains. Open Practices Open Science: This manuscript was awarded with the Open Materials Badge. For more information see: https://cos.io/our-services/open-science-badges/
机译:摘要帕金森病(Pd) - 富含幼亮的重复激酶2(LRRK 2)属于罗科家族的G-蛋白,其包含络合物(ROC)结构域,然后是ROC(COR)的C末端域名串联(称为roc-cor域)。两种原核毒素结构域的表征为鸟嘌呤核苷酸依赖性二聚化(GAD S)激活的G蛋白,这需要二聚化以激活它们的GTP ASE活性并结合具有相对低亲和力的鸟嘌呤核苷酸。另外,LRRK 2 ROC结构域分离地结合具有相对低亲和力的鸟嘌呤核苷酸。因此,预计LRRK 2 GTP ASE域将是一个GAD。在此,我们描述了人LRRK 2 Roc-Cor结构域的设计和高级表达(LRRK 2 Roc-Cor)。 LRRK 2 Roc-Cor的生化分析表明它形成同型二聚体,Cy的C末端部分介导其二聚化。此外,它在1?:1个化学计量中共净化并结合Mg 2+ GTP / GDP,并用K m水解GTP?和? K猫? 22 nm和4.70?×10?4?min?1,?分别。因此,即使LRRK 2 Roc-Cor形成GAD-like同源体,它也表现出常规的RA样GTP ASE性质,具有Mg 2+ - GTP / GDP和低固有催化活性的高亲和力结合。先前据报道,映射到COR结构域的PD加入Y1699C突变以减少全长LRRK的GTP ASE活性。相反,该突变在GTP ASE活动中诱导没有变化,并且在二级结构内容中只有轻微的扰动LRRK 2 Roc-Cor。由于该突变不直接影响分离的Roc-Cor串联的GTP ASE活性,因此可以通过其他功能域发生这种突变对全长LRRK 2的影响。开放实践公开科学:此手稿是授予开放材料徽章的奖励。有关更多信息,请参阅:https://cos.io/our-services/open-science-badges/

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