首页> 美国卫生研究院文献>Protein Science : A Publication of the Protein Society >Modulation of kinase-inhibitor interactions by auxiliary protein binding: Crystallography studies on Aurora A interactions with VX-680 and with TPX2
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Modulation of kinase-inhibitor interactions by auxiliary protein binding: Crystallography studies on Aurora A interactions with VX-680 and with TPX2

机译:辅助蛋白结合对激酶-抑制剂相互作用的调节:Aurora A与VX-680和TPX2相互作用的晶体学研究

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摘要

VX-680, also known as MK-0457, is an ATP-competitive small molecule inhibitor of the Aurora kinases that has entered phase II clinical trials for the treatment of cancer. We have solved the cocrystal structure of AurA/TPX2/VX-680 at 2.3 Å resolution. In the crystal structure, VX-680 binds to the active conformation of AurA. The glycine-rich loop in AurA adopts a unique bent conformation, forming a π–π interaction with the phenyl group of VX-680. In contrast, in the published AurA/VX-680 structure, VX-680 binds to AurA in the inactive conformation, interacting with a hydrophobic pocket only present in the inactive conformation. These data suggest that TPX2, a protein cofactor, can alter the binding mode of VX-680 with AurA. More generally, the presence of physiologically relevant cofactor proteins can alter the kinetics, binding interactions, and inhibition of enzymes, and studies with these multiprotein complexes may be beneficial to the discovery and optimization of enzyme inhibitors as therapeutic agents.
机译:VX-680,也称为MK-0457,是Aurora激酶的ATP竞争性小分子抑制剂,已进入II期临床试验以治疗癌症。我们已经解决了分辨率为2.3Å的AurA / TPX2 / VX-680的共晶体结构。在晶体结构中,VX-680与AurA的活性构象结合。 AurA中富含甘氨酸的环采用独特的弯曲构象,与VX-680的苯基形成π-π相互作用。相反,在公开的AurA / VX-680结构中,VX-680以非活性构象与AurA结合,与仅存在于非活性构象中的疏水口袋相互作用。这些数据表明,蛋白质辅助因子TPX2可以改变VX-680与AurA的结合模式。更一般地,生理相关辅因子蛋白的存在可以改变酶的动力学,结合相互作用和抑制,并且对这些多蛋白复合物的研究可能有利于发现和优化作为治疗剂的酶抑制剂。

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