Synthesis and Identification of New N,N-Disubstituted Thiourea, and Thiazolidinone Scaffolds Based on Quinolone Moiety as Urease Inhibitor

Synthesis of thiazolidinone based on quinolone moiety was established starting from 4-hydroxyquinol-2-ones. The strategy started with the reaction of ethyl bromoacetate with 4-hydroxyquinoline to give the corresponding ethyl oxoquinolinyl acetates, which reacted with hydrazine hydrate to afford the...

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Published inMolecules (Basel, Switzerland) Vol. 27; no. 20; p. 7126
Main Authors Elshaier, Yaseen A. M. M., Aly, Ashraf A., Abdel-Aziz, Mohamed, Fathy, Hazem M., Brown, Alan B., Bräse, Stefan, Ramadan, Mohamed
Format Journal Article
LanguageEnglish
Published Basel MDPI AG 21.10.2022
MDPI
Subjects
Acetates
Acetic acid
Acids
Bacteria
Cancer
dialkyl acetylenedicarboxylates
Enzymes
Hydrazides
Hydrazine
Hydrazines
Hydroxyquinoline
in vitro urease inhibition properties
Inhibitors
Isothiocyanate
Microorganisms
Molecular docking
N,N-disubstituted thioureas
Nitrogen
thiazolidinones
Thiourea
Thioureas
Urease
Urogenital system
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Summary:Synthesis of thiazolidinone based on quinolone moiety was established starting from 4-hydroxyquinol-2-ones. The strategy started with the reaction of ethyl bromoacetate with 4-hydroxyquinoline to give the corresponding ethyl oxoquinolinyl acetates, which reacted with hydrazine hydrate to afford the hydrazide derivatives. Subsequently, hydrazides reacted with isothiocyanate derivatives to give the corresponding N,N-disubstituted thioureas. Finally, on subjecting the N,N-disubstituted thioureas with dialkyl acetylenedicarboxylates, cyclization occurred, and thiazolidinone derivatives were obtained in good yields. The two series based on quinolone moiety, one containing N,N-disubstituted thioureas and the other containing thiazolidinone functionalities, were screened for their in vitro urease inhibition properties using thiourea and acetohydroxamic acid as standard inhibitors. The inhibition values of the synthesized thioureas and thiazolidinones exhibited moderate to good inhibitory effects. The structure−activity relationship revealed that N-methyl quinolonyl moiety exhibited a superior effect, since it was proved to be the most potent inhibitor in the present series achieving (IC50 = 1.83 ± 0.79 µM). The previous compound exhibited relatively much greater activity, being approximately 12-fold more potent than thiourea and acetohydroxamic acid as references. Molecular docking analysis showed a good protein−ligand interaction profile against the urease target (PDBID: 4UBP), emphasizing the electronic and geometric effect of N,N-disubstituted thiourea.
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ISSN:1420-3049
1420-3049
DOI:10.3390/molecules27207126