Discovery of novel 1,4-dicarbonylthiosemicarbazides as DNA gyrase inhibitors for the treatment of MRSA infection

bioRxiv - Pharmacology and Toxicology Pub Date : 2024-09-10 DOI:10.1101/2024.09.05.611349

Gao Zhang, Jiaxin Liang, Gang Wen, Mingli Yao, Yuqing Jia, Bo Feng, Jishun Li, Zunsheng Han, Qingxin Liu, Tianlei Li, Wenxuan Zhang, Hongwei Jin, Jie Xia, Liang Peng, Song Wu

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Abstract

Antibiotic resistance has become a serious threat to public health, thus novel antibiotics are urgently needed to combat drug-resistant bacteria including MRSA (methicillin-resistant S. aureus). The 1,4-dicarbonylthiosemicarbazide is an interesting chemotype that could exhibit antibacterial activity. However, the currently available compounds are not as potent as clinical antibiotics. Herein, we adopted the computer-aided drug design strategy, substructure search, to retrieve antibacterial 1,4-dicarbonylthiosemicarbazide derivatives, and identified compound B5 (Specs ID: AG-690/15432331) from the Specs chemical library that exhibited moderate activity (minimum inhibitory concentration (MIC): 6.25 μg/mL) against S. aureus (ATCC 29213). Based on that compound, we further designed and synthesized 45 derivatives, and evaluated their antibacterial activity. Eight derivatives were more potent than or equivalent to vancomycin (MIC: 1.56 μg/mL). We compared the three most potent ones for their cytotoxicity to HepG2 and HUVEC cells and selected compound 1b as our lead compound for comprehensive biological evaluation. As a result, compound 1b exhibited a bacteriostatic mode, and was active against a panel of gram-positive bacteria strains, metabolically stable, and effective to protect the mice from MRSA infection. More importantly, we applied 2D similarity calculation and reverse docking to predict potential targets of compound 1b. Through experimental validation and molecular dynamics simulation, we were able to confirm that compound 1b inhibited S. aureus DNA gyrase (IC50: 1.81 μM) and DNA supercoiling, potentially by binding to the ATPase domain, where ASP81, GLU58 and GLN91 formed key hydrogen bonds. Taken together, we have discovered a new class of DNA gyrase inhibitors represented by compound 1b for the treatment of MRSA infection, through the design, synthesis, and biological evaluation of novel 1,4-dicarbonylthiosemicarbazides.

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发现新型 1,4-二羰基硫代氨基甲酸盐作为 DNA 回旋酶抑制剂用于治疗 MRSA 感染

抗生素耐药性已严重威胁到公众健康，因此迫切需要新型抗生素来对抗包括 MRSA（耐甲氧西林金黄色葡萄球菌）在内的耐药细菌。1,4-二羰基硫代氨基甲酰肼是一种有趣的化学类型，可以表现出抗菌活性。然而，目前可用的化合物并不像临床抗生素那样有效。在此，我们采用计算机辅助药物设计策略--子结构搜索来检索抗菌的 1,4-二羰基氨基硫脲衍生物，并从 Specs 化学文库中发现了化合物 B5（Specs ID：AG-690/15432331），该化合物具有中等活性（最小抑菌浓度 (MIC)：6.25 μ/mL）：6.25 μg/mL）。在该化合物的基础上，我们进一步设计合成了 45 种衍生物，并评估了它们的抗菌活性。有 8 种衍生物的抗菌活性高于或等同于万古霉素（MIC：1.56 μg/mL）。我们比较了三种最有效的衍生物对 HepG2 和 HUVEC 细胞的细胞毒性，并选择化合物 1b 作为先导化合物进行全面的生物学评估。结果表明，化合物 1b 具有抑菌作用，对一系列革兰氏阳性菌株有活性，代谢稳定，能有效保护小鼠免受 MRSA 感染。更重要的是，我们应用二维相似性计算和反向对接预测了化合物 1b 的潜在靶点。通过实验验证和分子动力学模拟，我们证实化合物 1b 能抑制金黄色葡萄球菌 DNA 回旋酶（IC50：1.81 μM）和 DNA 超卷曲，可能是通过与 ATPase 结构域结合，其中 ASP81、GLU58 和 GLN91 形成了关键的氢键。综上所述，我们通过设计、合成和生物学评价新型 1,4-二羰基硫代氨基脲，发现了以化合物 1b 为代表的一类新的 DNA 回旋酶抑制剂，可用于治疗 MRSA 感染。

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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bioRxiv - Pharmacology and Toxicology

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