| Literature DB >> 30571121 |
Carlos Moreno-Cinos1, Elisa Sassetti2,3, Irene G Salado1, Gesa Witt2, Siham Benramdane1, Laura Reinhardt4, Cristina D Cruz5, Jurgen Joossens1, Pieter Van der Veken1, Heike Brötz-Oesterhelt4, Päivi Tammela5, Mathias Winterhalter3, Philip Gribbon2, Björn Windshügel2, Koen Augustyns1.
Abstract
Increased Gram-negative bacteria resistance to antibiotics is becoming a global problem, and new classes of antibiotics with novel mechanisms of action are required. The caseinolytic protease subunit P (ClpP) is a serine protease conserved among bacteria that is considered as an interesting drug target. ClpP function is involved in protein turnover and homeostasis, stress response, and virulence among other processes. The focus of this study was to identify new inhibitors of Escherichia coli ClpP and to understand their mode of action. A focused library of serine protease inhibitors based on diaryl phosphonate warheads was tested for ClpP inhibition, and a chemical exploration around the hit compounds was conducted. Altogether, 14 new potent inhibitors of E. coli ClpP were identified. Compounds 85 and 92 emerged as most interesting compounds from this study due to their potency and, respectively, to its moderate but consistent antibacterial properties as well as the favorable cytotoxicity profile.Entities:
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Year: 2019 PMID: 30571121 DOI: 10.1021/acs.jmedchem.8b01466
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446