首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Crystal Structures of the Scaffolding Protein LGN Reveal the General Mechanism by Which GoLoco Binding Motifs Inhibit the Release of GDP from Gαi
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Crystal Structures of the Scaffolding Protein LGN Reveal the General Mechanism by Which GoLoco Binding Motifs Inhibit the Release of GDP from Gαi

机译:支架蛋白LGN的晶体结构揭示了GoLoco结合基序抑制GDP从Gαi释放的一般机制。

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摘要

GoLoco (GL) motif-containing proteins regulate G protein signaling by binding to Gα subunit and acting as guanine nucleotide dissociation inhibitors. GLs of LGN are also known to bind the GDP form of Gαi/o during asymmetric cell division. Here, we show that the C-terminal GL domain of LGN binds four molecules of Gαi·GDP. The crystal structures of Gαi·GDP in complex with LGN GL3 and GL4, respectively, reveal distinct GL/Gαi interaction features when compared with the only high resolution structure known with GL/Gαi interaction between RGS14 and Gαi1. Only a few residues C-terminal to the conserved GL sequence are required for LGN GLs to bind to Gαi·GDP. A highly conserved “double Arg finger” sequence (RΨ(D/E)(D/E)QR) is responsible for LGN GL to bind to GDP bound to Gαi. Together with the sequence alignment, we suggest that the LGN GL/Gαi interaction represents a general binding mode between GL motifs and Gαi. We also show that LGN GLs are potent guanine nucleotide dissociation inhibitors.
机译:包含GoLoco(GL)基序的蛋白质通过与Gα亚基结合并充当鸟嘌呤核苷酸解离抑制剂来调节G蛋白信号传导。还已知LGN的GL在不对称细胞分裂过程中结合Gαi/ o的GDP形式。在这里,我们显示LGN的C末端GL域结合了四个Gαi·GDP分子。与已知只有RGS14和Gαi1之间发生GL /Gαi相互作用的高分辨率结构相比,分别与LGN GL3和GL4复合的Gαi·GDP的晶体结构显示出独特的GL /Gαi相互作用特征。 LGN GL与Gαi·GDP结合只需要保守的GL序列C末端的几个残基。高度保守的“双Arg指”序列(RΨ(D / E)(D / E)QR)导致LGN GL与绑定到Gαi的GDP结合。连同序列比对,我们建议LGN GL /Gαi相互作用代表了GL基序和Gαi之间的一般结合方式。我们还表明,LGN GLs是有效的鸟嘌呤核苷酸解离抑制剂。

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