靶向蛋白激酶特定无活性形式的亲和试剂。
Affinity reagents that target a specific inactive form of protein kinases.
作者信息
Ranjitkar Pratistha, Brock Amanda M, Maly Dustin J
机构信息
Department of Chemistry, University of Washington, Seattle, WA 98195, USA.
出版信息
Chem Biol. 2010 Feb 26;17(2):195-206. doi: 10.1016/j.chembiol.2010.01.008.
Abstract
A number of small-molecule inhibitors have been developed that target the catalytic domains of protein kinases that are not in an active conformation. An inactive form that has been observed in several kinases is the DFG-out conformation. This conformation is characterized by an almost 180 degrees rotation of the conserved Asp-Phe-Gly (DFG) motif in the ATP-binding cleft relative to the active form. However, the sequence and structural determinants that allow a kinase to stably adopt the DFG-out conformation are not known. Here, we characterize a series of inhibitors based on a general pharmacophore for this inactive form. We demonstrate that modified versions of these inhibitors can be used to study the thermodynamics and kinetics of ligand binding to DFG-out-adopting kinases and for enriching these kinases from complex protein mixtures.
摘要
已经开发出许多靶向处于非活性构象的蛋白激酶催化结构域的小分子抑制剂。在几种激酶中观察到的一种非活性形式是DFG-out构象。这种构象的特征是,相对于活性形式,ATP结合裂隙中保守的天冬氨酸-苯丙氨酸-甘氨酸(DFG)基序发生了近180度的旋转。然而,使激酶稳定采用DFG-out构象的序列和结构决定因素尚不清楚。在这里,我们基于这种非活性形式的通用药效团来表征一系列抑制剂。我们证明,这些抑制剂的修饰版本可用于研究配体与采用DFG-out构象的激酶结合的热力学和动力学,以及从复杂的蛋白质混合物中富集这些激酶。
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