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Antimycobacterial pyridine carboxamides: From design to in vivo activity

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Author
Nawrot, Daria Elżbieta
Bouz, GhadaORCiD Profile - 0000-0003-2024-5788WoS Profile - S-6361-2017Scopus Profile - 57195723273
Janďourek, OndřejORCiD Profile - 0000-0003-4633-2062WoS Profile - S-7884-2017Scopus Profile - 56016528500
Konečná, KláraORCiD Profile - 0000-0001-5670-7767WoS Profile - S-9399-2017Scopus Profile - 37052510300
Paterová, PavlaORCiD Profile - 0000-0003-0192-7345WoS Profile - L-6100-2017Scopus Profile - 55504598600
Bárta, PavelORCiD Profile - 0000-0001-5445-5658WoS Profile - S-5613-2017Scopus Profile - 49662783000
Novák, Martin
Kučera, RadimORCiD Profile - 0000-0003-3052-7965WoS Profile - S-6366-2017Scopus Profile - 56250821200
Zemanová, Júlia
Forbak, Martin
Korduláková, Jana
Pavliš, Oto
Kubíčková, Pavla
Doležal, MartinORCiD Profile - 0000-0003-1558-6625WoS Profile - N-8860-2013Scopus Profile - 7006495068
Zitko, JanORCiD Profile - 0000-0003-0104-9925WoS Profile - G-3442-2012Scopus Profile - 6508128302

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Publication date
2023
Published in
European Journal of Medicinal Chemistry
Volume / Issue
258 (October)
ISBN / ISSN
ISSN: 0223-5234
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  • Faculty of Pharmacy in Hradec Králové

This publication has a published version with DOI 10.1016/j.ejmech.2023.115617

Abstract
Tuberculosis is the number one killer of infectious diseases caused by a single microbe, namely Mycobacterium tuberculosis (Mtb). The success rate of curing this infection is decreasing due to emerging antimicrobial resistance. Therefore, novel treatments are urgently needed. As an attempt to develop new antituberculars effective against both drugs-sensitive and drug-resistant Mtb, we report the synthesis of a novel series inspired by combining fragments from the first-line agents isoniazid and pyrazinamide (series I) and isoniazid with the second-line agent 4-aminosalicylic acid (series II). We identified compound 10c from series II with selective, potent in vitro antimycobacterial activity against both drug-sensitive and drug-resistant Mtb H37Rv strains with no in vitro or in vivo cytotoxicity. In the murine model of tuberculosis, compound 10c caused a statistically significant decrease in colony-forming units (CFU) in spleen. Despite having a 4-aminosalicylic acid fragment in its structure, biochemical studies showed that compound 10c does not directly affect the folate pathway but rather methionine metabolism. In silico simulations indicated the possibility of binding to mycobacterial methionine-tRNA synthetase. Metabolic study in human liver microsomes revealed that compound 10c does not have any known toxic metabolites and has a half-life of 630 min, overcoming the main drawbacks of isoniazid (toxic metabolites) and 4-aminosalicylic acid (short half-life).
Keywords
4-Aminosalicylic acid, Isoniazid, Multidrug-resistance, Pyrazinamide, Pyridine, Tuberculosis
Permanent link
https://hdl.handle.net/20.500.14178/1977
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WOS:001039259300001
SCOPUS:2-s2.0-85164325465
PUBMED:37423128
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