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处于活性和非活性构象的人类Rab4a的高分辨率晶体结构。

High resolution crystal structures of human Rab4a in its active and inactive conformations.

作者信息

Huber Silke K, Scheidig Axel J

机构信息

Max-Planck Institut für Molekulare Physiologie, Abteilung für Physikalische Biochemie, Dortmund, Germany.

出版信息

FEBS Lett. 2005 May 23;579(13):2821-9. doi: 10.1016/j.febslet.2005.04.020. Epub 2005 Apr 25.

DOI:10.1016/j.febslet.2005.04.020
PMID:15907487
Abstract

The Ras-related human GTPase Rab4a is involved in the regulation of endocytosis through the sorting and recycling of early endosomes. Towards further insight, we have determined the three-dimensional crystal structure of human Rab4a in its GppNHp-bound state to 1.6 Angstroms resolution and in its GDP-bound state to 1.8 Angstroms resolution, respectively. Despite the similarity of the overall structure with other Rab proteins, Rab4a displays significant differences. The structures are discussed with respect to the recently determined structure of human Rab5a and its complex with the Rab5-binding domain of the bivalent effector Rabaptin-5. The Rab4 specific residue His39 modulates the nucleotide binding pocket giving rise to a reduced rate for nucleotide hydrolysis and exchange. In comparison to Rab5, Rab4a has a different GDP-bound conformation within switch 1 region and displays shifts in position and orientation of the hydrophobic triad. The observed differences at the S2-L3-S3 region represent a new example of structural plasticity among Rab proteins and may provide a structural basis to understand the differential binding of similar effector proteins.

摘要

与Ras相关的人类GTP酶Rab4a通过早期内体的分选和再循环参与内吞作用的调控。为了进一步深入了解,我们分别确定了处于结合GppNHp状态的人类Rab4a的三维晶体结构,分辨率为1.6埃,以及处于结合GDP状态的人类Rab4a的三维晶体结构,分辨率为1.8埃。尽管Rab4a的整体结构与其他Rab蛋白相似,但它仍表现出显著差异。结合最近确定的人类Rab5a及其与二价效应器Rabaptin-5的Rab5结合结构域的复合物的结构,对这些结构进行了讨论。Rab4特有的残基His39调节核苷酸结合口袋,导致核苷酸水解和交换速率降低。与Rab5相比,Rab4a在开关1区域内具有不同的结合GDP的构象,并且疏水三联体的位置和方向发生了变化。在S2-L3-S3区域观察到的差异代表了Rab蛋白之间结构可塑性的一个新例子,可能为理解相似效应蛋白的差异结合提供结构基础。

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