了解磷酸化在PDZ结构域结合机制中的作用

A. Toto, A. Mattei, P. Jemth, S. Gianni
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引用次数: 15

摘要

PDZ结构域是哺乳动物中最常见的蛋白-蛋白相互作用结构域之一。虽然一些研究已经证明了磷酸化在涉及PDZ结构域的相互作用中的重要性,但缺乏详细的机制数据来解决磷酸化如何影响PDZ相互作用。在这里,我们通过平衡和动力学结合实验解决了这个问题,利用蛋白酪氨酸磷酸酶L1的PDZ2及其与天然配体RIL的肽的相互作用。结果表明,RIL肽中丝氨酸残基的磷酸化具有双重和相反的作用:它增加了结合和解离速率常数,从而导致结合的整体减弱。此外,我们对RIL肽进行了结合实验,其中丝氨酸被谷氨酸取代,这是一种常用的模拟蛋白质磷酸化的方法。引人注目的是,无论是亲和力和离子强度依赖的亲和力的磷酸丝氨酸和谷氨酸肽明显不同。这些结果表明,在这种特殊情况下,谷氨酸是一种很差的丝氨酸磷酸化模拟物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Understanding the role of phosphorylation in the binding mechanism of a PDZ domain
The PDZ domain is one of the most common protein–protein interaction domains in mammalian species. While several studies have demonstrated the importance of phosphorylation in interactions involving PDZ domains, there is a paucity of detailed mechanistic data addressing how the PDZ interaction is affected by phosphorylation. Here, we address this question by equilibrium and kinetic binding experiments using PDZ2 from protein tyrosine phosphatase L1 and its interaction with a peptide from the natural ligand RIL. The results show that phosphorylation of a serine residue in the RIL peptide has dual and opposing effects: it increases both the association and dissociation rate constants, which leads to an overall weakening of binding. Furthermore, we performed binding experiments with a RIL peptide in which the serine was replaced by a glutamate, a commonly used method to mimic phosphorylation in proteins. Strikingly, both the affinity and the ionic strength dependence of the affinity differed markedly for the phosphoserine and glutamate peptides. These results show that, in this particular case, glutamate is a poor mimic of serine phosphorylation.
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