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首页> 外文期刊>Journal of Molecular Biology >Allosteric Modulation of Binding Specificity by Alternative Packing of Protein Cores
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Allosteric Modulation of Binding Specificity by Alternative Packing of Protein Cores

机译:蛋白质核心替代包装结合特异性的变构调节

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摘要

Hydrophobic cores are often viewed as tightly packed and rigid, but they do show some plasticity and could thus be attractive targets for protein design. Here we explored the role of different functional pressures on the core packing and ligand recognition of the SH3 domain from human Fyn tyrosine kinase. We randomized the hydrophobic core and used phage display to select variants that bound to each of three distinct ligands. The three evolved groups showed remarkable differences in core composition, illustrating the effect of different selective pressures on the core. Changes in the core did not significantly alter protein stability, but were linked closely to changes in binding affinity and specificity. Structural analysis and molecular dynamics simulations revealed the structural basis for altered specificity. The evolved domains had significantly reduced core volumes, which in turn induced increased backbone flexibility. These motions were propagated from the core to the binding surface and induced significant conformational changes. These results show that alternative core packing and consequent allosteric modulation of binding interfaces could be used to engineer proteins with novel functions. Crown Copyright (C) 2018 Published by Elsevier Ltd. All rights reserved.
机译:疏水性核心通常被视为紧密填充和刚性,但它们确实表现出一些可塑性,因此可以是蛋白质设计的吸引力。在这里,我们探讨了不同功能压力对来自人Fyn酪氨酸激酶的SH3结构域的核心包装和配体识别的作用。我们随机化疏水芯和使用噬菌体展示,选择与三个不同配体中的每一个结合的变体。三个进化的基团显示出核心组合物的显着差异,说明了不同选择性压力对芯的影响。核心的变化没有显着改变蛋白质稳定性,但与结合亲和力和特异性的变化密切相关。结构分析和分子动力学模拟显示出改变特异性的结构基础。进化的域具有显着降低的核心体积,这反过来诱导增加的骨干柔性。这些运动从核心传播到结合表面,并诱导显着的构象变化。这些结果表明,替代核心包装和结合结合界面的变构调制可用于用新颖功能工程蛋白。 Crown版权(c)2018由elestvier有限公司出版。保留所有权利。

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