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首页> 外文期刊>Journal of molecular recognition: JMR >Modeling the interaction between the N-terminal domain of the tumor suppressor p53 and azurin.
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Modeling the interaction between the N-terminal domain of the tumor suppressor p53 and azurin.

机译:模拟肿瘤抑制因子p53的N末端结构域与天青蛋白之间的相互作用。

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It is known that the half life of the tumor suppressor p53 can be increased by the interaction with the bacterial protein azurin, resulting in an enhanced anti-tumoral activity. The understanding of the molecular mechanisms on the basis of this phenomenon can open the way to new anti-cancer strategies. Some experimental works have given evidence of an interaction between p53 and azurin (AZ); however the binding regions of the proteins are still unknown. Recently, fluorescence studies have shown that p53 partakes in the binding with the bacterial protein by its N-terminal (NT) domain. Here we have used a computational method to get insight into this interacting mode. The model that we propose for the best complex between AZ and p53 has been obtained from a rigid-body docking, coupled with a molecular dynamics (MD) simulation, a free energy calculation, and validated by mutagenesis analysis. We have found a high degree of geometric fit between the two proteins that are kept together by several hydrophobic interactions and numerous hydrogen bonds. Interestingly, it has emerged that AZ binds essentially to the helices H(I) and H(III) of the p53 NT domain, which are also interacting regions for the foremost inhibitor of p53, MDM2.
机译:已知通过与细菌蛋白天青蛋白的相互作用可以增加抑癌基因p53的半衰期,从而提高抗肿瘤活性。基于这种现象的分子机制的理解可以为新的抗癌策略开辟道路。一些实验工作已经提供了p53和azurin(AZ)之间相互作用的证据。然而,蛋白质的结合区域仍然未知。最近,荧光研究表明,p53通过其N端(NT)域参与与细菌蛋白的结合。在这里,我们使用了一种计算方法来深入了解这种交互模式。我们建议的AZ和p53之间最佳复杂度的模型是通过刚体对接获得的,结合了分子动力学(MD)模拟,自由能计算,并通过诱变分析进行了验证。我们已经发现了两种蛋白质之间的高度几何拟合,这些蛋白质通过几个疏水相互作用和许多氢键保持在一起。有趣的是,已经发现AZ基本上与p53 NT域的螺旋H(I)和H(III)结合,它们也是p53最重要的抑制剂MDM2的相互作用区域。

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