Discovery and Hit-to-Lead Optimization of Benzothiazole Scaffold- Based DNA Gyrase Inhibitors with Potent Activity against Acinetobacter baumannii and Pseudomonas aeruginosa

被引:24
作者
Cotman, Andrej Emanuel [1 ]
Durcik, Martina [1 ]
Tiz, Davide Benedetto [1 ,2 ]
Fulgheri, Federica [1 ,3 ]
Secci, Daniela [1 ,3 ]
Sterle, Masa [1 ]
Mozina, Stefan [1 ,4 ]
Skok, Ziga [1 ,4 ]
Zidar, Nace [1 ]
Zega, Anamarija [1 ]
Ilas, Janez [1 ]
Masic, Lucija Peterlin [1 ]
Tomasic, Tihomir [1 ]
Hughes, Diarmaid [5 ]
Huseby, Douglas L. [5 ]
Cao, Sha [5 ]
Garoff, Linnea [5 ]
Fernandez, Talia Berruga [5 ]
Giachou, Paraskevi [5 ]
Crone, Lisa [5 ]
Simoff, Ivailo [6 ]
Svensson, Richard [6 ]
Birnir, Bryndis [7 ]
Korol, Sergiy V. [7 ]
Jin, Zhe [7 ]
Vicente, Francisca [8 ]
Ramos, Maria C. [8 ]
de la Cruz, Mercedes [8 ]
Glinghammar, Bjorn [9 ]
Lenhammar, Lena [11 ]
Henderson, Sara R. [10 ,12 ]
Mundy, Julia E. A. [10 ]
Maxwell, Anthony [10 ]
Stevenson, Clare E. M. [10 ]
Lawson, David M. [10 ]
Janssen, Guido V.
Sterk, Geert Jan
Kikelj, Danijel [1 ]
机构
[1] Univ Ljubljana, Fac Pharm, Ljubljana 1000, Slovenia
[2] Univ Perugia, Dept Pharmaceut Sci, Via Liceo 1, I-06100 Perugia, Italy
[3] Univ Cagliari, Dept Life & Environm Sci, Drug Sect, Via Osped 72, I-09124 Cagliari, Italy
[4] Lek Pharmaceut, Verovskova Ul 57, Ljubljana 1000, Slovenia
[5] Uppsala Univ, Dept Med Biochem & Microbiol, S-75123 Uppsala, Sweden
[6] Uppsala Univ, Dept Pharm, Drug Optimizat & Pharmaceut Profiling Platform UDO, S-75123 Uppsala, Sweden
[7] Uppsala Univ, Dept Med Cell Biol, S-75123 Uppsala, Sweden
[8] Fundac MEDINA, Granada 18016, Spain
[9] RISE Res Inst Sweden, Dept Chem Proc & Pharmaceut Dev, Unit Chem & Pharmaceut Safety, S-15136 Sodertalje, Sweden
[10] John Innes Ctr, Dept Biochem & Metab, Norwich NR4 7UH, England
[11] Uppsala Univ Hosp, Dept Med Sci, S-75185 Uppsala, Sweden
[12] Univ Birmingham, Inst Microbiol & Infect, Coll Med & Dent Sci, Birmingham, England
基金
英国生物技术与生命科学研究理事会; 英国惠康基金;
关键词
DRUG DISCOVERY; ANTAGONISTS;
D O I
10.1021/acs.jmedchem.2c01597
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We have developed compounds with a promising activity against Acinetobacter baumannii and Pseudomonas aerugi-nosa, which are both on the WHO priority list of antibiotic -resistant bacteria. Starting from DNA gyrase inhibitor 1, we identified compound 27, featuring a 10-fold improved aqueous solubility, a 10-fold improved inhibition of topoisomerase IV from A. baumannii and P. aeruginosa, a 10-fold decreased inhibition of human topoisomerase II alpha, and no cross-resistance to novobiocin. Cocrystal structures of 1 in complex with Escherichia coli GyrB24 and (S)-27 in complex with A. baumannii GyrB23 and P. aeruginosa GyrB24 revealed their binding to the ATP-binding pocket of the GyrB subunit. In further optimization steps, solubility, plasma free fraction, and other ADME properties of 27 were improved by fine-tuning of lipophilicity. In particular, analogs of 27 with retained anti-Gram-negative activity and improved plasma free fraction were identified. The series was found to be nongenotoxic, nonmutagenic, devoid of mitochondrial toxicity, and possessed no ion channel liabilities.
引用
收藏
页码:1380 / 1425
页数:46
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