水网络在磷酸二酯酶抑制剂解离和动力学选择性中的作用

IF 3.6 4区 医学 Q2 CHEMISTRY, MEDICINAL
ChemMedChem Pub Date : 2024-08-28 DOI:10.1002/cmdc.202400417
Antoni R Blaazer, Abhimanyu K Singh, Lorena Zara, Pierre Boronat, Lady J Bautista, Steve Irving, Maciej Majewski, Xavier Barril, Maikel Wijtmans, U Helena Danielson, Geert Jan Sterk, Rob Leurs, Jacqueline E van Muijlwijk-Koezen, David G Brown, Iwan de Esch
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引用次数: 0

摘要

为了寻找开发对非目标人类 PDE4(hPDE4)具有选择性的布氏锥虫磷酸二酯酶 B1(TbrPDEB1)抑制剂的新机会,研究人员利用各种生化、结构、热力学和动力学结合试验对片段生长活动的不同阶段进行了研究。研究发现了结合动力学的显著差异,并通过计算方法(包括分子动力学和相互作用指纹分析)对这种动力学选择性进行了探索。这些研究表明,GlnQ.50 与抑制剂之间的一个关键氢键暴露于 TbrPDEB1 的水通道中,导致快速解除结合。hPDE4 中不存在这种水通道,因此抑制剂的停留时间较长。我们将计算机辅助药物设计方案应用于最近公开的一种具有不同支架的 TbrPDEB1 抑制剂,结果证实,通过破坏水通道来屏蔽这一关键氢键是开发更具选择性的 TbrPDEB1 抑制剂的一种可行的设计策略。我们的工作表明了如何利用计算协议来了解溶剂动力学对抑制剂结合的贡献,我们的结果可用于设计相关寄生虫中同源 PDE 的选择性抑制剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The Role of Water Networks in Phosphodiesterase Inhibitor Dissociation and Kinetic Selectivity.

In search of new opportunities to develop Trypanosoma brucei phosphodiesterase B1 (TbrPDEB1) inhibitors that have selectivity over the off-target human PDE4 (hPDE4), different stages of a fragment-growing campaign were studied using a variety of biochemical, structural, thermodynamic, and kinetic binding assays. Remarkable differences in binding kinetics were identified and this kinetic selectivity was explored with computational methods, including molecular dynamics and interaction fingerprint analyses. These studies indicate that a key hydrogen bond between GlnQ.50 and the inhibitors is exposed to a water channel in TbrPDEB1, leading to fast unbinding. This water channel is not present in hPDE4, leading to inhibitors with a longer residence time. The computer-aided drug design protocols were applied to a recently disclosed TbrPDEB1 inhibitor with a different scaffold and our results confirm that shielding this key hydrogen bond through disruption of the water channel represents a viable design strategy to develop more selective inhibitors of TbrPDEB1. Our work shows how computational protocols can be used to understand the contribution of solvent dynamics to inhibitor binding, and our results can be applied in the design of selective inhibitors for homologous PDEs found in related parasites.

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来源期刊
ChemMedChem
ChemMedChem 医学-药学
CiteScore
6.70
自引率
2.90%
发文量
280
审稿时长
1 months
期刊介绍: Quality research. Outstanding publications. With an impact factor of 3.124 (2019), ChemMedChem is a top journal for research at the interface of chemistry, biology and medicine. It is published on behalf of Chemistry Europe, an association of 16 European chemical societies. ChemMedChem publishes primary as well as critical secondary and tertiary information from authors across and for the world. Its mission is to integrate the wide and flourishing field of medicinal and pharmaceutical sciences, ranging from drug design and discovery to drug development and delivery, from molecular modeling to combinatorial chemistry, from target validation to lead generation and ADMET studies. ChemMedChem typically covers topics on small molecules, therapeutic macromolecules, peptides, peptidomimetics, and aptamers, protein-drug conjugates, nucleic acid therapies, and beginning 2017, nanomedicine, particularly 1) targeted nanodelivery, 2) theranostic nanoparticles, and 3) nanodrugs. Contents ChemMedChem publishes an attractive mixture of: Full Papers and Communications Reviews and Minireviews Patent Reviews Highlights and Concepts Book and Multimedia Reviews.
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