Structure-Based Design and Development of Phosphine Oxides as a Novel Chemotype for Antibiotics that Dysregulate Bacterial ClpP Proteases.

IF 6.8 1区医学 Q1 CHEMISTRY, MEDICINAL

Journal of Medicinal Chemistry Pub Date : 2024-09-12 Epub Date: 2024-09-02 DOI:10.1021/acs.jmedchem.4c00773

Funing Lin, Mark F Mabanglo, Jin Lin Zhou, Gursonika Binepal, Marim M Barghash, Keith S Wong, Scott D Gray-Owen, Robert A Batey, Walid A Houry

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Abstract

A series of arylsulfones and heteroarylsulfones have previously been demonstrated to dysregulate the conserved bacterial ClpP protease, causing the unspecific degradation of essential cellular housekeeping proteins and ultimately resulting in cell death. A cocrystal structure of a 2-β-sulfonylamide analog, ACP1-06, with Escherichia coli ClpP showed that its 2-pyridyl sulfonyl substituent adopts two orientations in the binding site related through a sulfone bond rotation. From this, a new bis-aryl phosphine oxide scaffold, designated as ACP6, was designed based on a "conformation merging" approach of the dual orientation of the ACP1-06 sulfone. One analog, ACP6-12, exhibited over a 10-fold increase in activity over the parent ACP1-06 compound, and a cocrystal X-ray structure with ClpP confirmed its predicted binding conformation. This allowed for a comparative analysis of how different ligand classes bind to the hydrophobic binding site. The study highlights the successful application of structure-based rational design of novel phosphine oxide-based antibiotics.

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以结构为基础设计和开发氧化膦，将其作为可抑制细菌 ClpP 蛋白酶的抗生素的新型化学类型。

一系列芳基砜和杂芳基砜先前已被证明能使保守的细菌 ClpP 蛋白酶失调，导致细胞重要的管家蛋白发生非特异性降解，最终导致细胞死亡。2-β 磺酰酰胺类似物 ACP1-06 与大肠杆菌 ClpP 的共晶体结构显示，其 2-吡啶基磺酰基取代基通过砜键旋转在结合位点采用了两种方向。由此，根据 ACP1-06 砜的双取向 "构象合并 "方法，设计出了一种新的双芳基氧化膦支架，命名为 ACP6。其中一种类似物 ACP6-12 的活性比 ACP1-06 母体化合物提高了 10 倍以上，与 ClpP 的共晶体 X 射线结构证实了其预测的结合构象。这样就可以对不同配体类别如何与疏水结合位点结合进行比较分析。该研究强调了基于结构的新型氧化膦抗生素合理设计的成功应用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Medicinal Chemistry 医学-医药化学

CiteScore

4.00

自引率

11.00%

发文量

804

审稿时长

1.9 months

期刊介绍： The Journal of Medicinal Chemistry is a prestigious biweekly peer-reviewed publication that focuses on the multifaceted field of medicinal chemistry. Since its inception in 1959 as the Journal of Medicinal and Pharmaceutical Chemistry, it has evolved to become a cornerstone in the dissemination of research findings related to the design, synthesis, and development of therapeutic agents. The Journal of Medicinal Chemistry is recognized for its significant impact in the scientific community, as evidenced by its 2022 impact factor of 7.3. This metric reflects the journal's influence and the importance of its content in shaping the future of drug discovery and development. The journal serves as a vital resource for chemists, pharmacologists, and other researchers interested in the molecular mechanisms of drug action and the optimization of therapeutic compounds.