Synthesis, urease inhibitory and anticancer evaluation of glucosamine-sulfonylurea conjugates

Urease catalyses the hydrolysis of urea to ammonia and carbon dioxide. This enzyme is important in the virulence of several human pathogens and urease activity in soil can cleave urea fertilisers prematurely, leading to waste of agricultural nitrogen. A series of arylsulfonylurea-glucosamine hybrid...

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Published inMedicinal chemistry research Vol. 33; no. 4; pp. 663 - 676
Main Authors Suaifan, Ghadeer A. R. Y., Shehadeh, Mayadah, Tahboub, Dua’a, Mohammed, Aya A. M., Threadgill, Michael D., Gaurav, Anand, Khan, Majid
Format Journal Article
LanguageEnglish
Published New York Springer US 01.04.2024
Springer Nature B.V
Subjects
Agricultural wastes
Agrochemicals
Ammonia
Biochemistry
Biomedical and Life Sciences
Biomedicine
Bioorganic Chemistry
Carbon dioxide
Chemical synthesis
Chloroformate
Cytotoxicity
Docking
Glucosamine
Hybrids
Inorganic Chemistry
Intermediates
Medicinal Chemistry
Methanolysis
N-Acetylglucosamine
Nitrogen
Original Research Article
Pharmacology/Toxicology
Renal cell carcinoma
Scavenging
Structure-activity relationships
Substitution reactions
Sulfonylurea
Ureas
Urease
Virulence
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Summary:Urease catalyses the hydrolysis of urea to ammonia and carbon dioxide. This enzyme is important in the virulence of several human pathogens and urease activity in soil can cleave urea fertilisers prematurely, leading to waste of agricultural nitrogen. A series of arylsulfonylurea-glucosamine hybrid compounds were synthesised. Reaction of arylsulfonamides with phenyl chloroformate and 4-dimethylaminopyridine gave either phenyl N-(2,4-arylsulfonyl)carbamate 4-dimethylaminopyridinium salts or N-(4-arylsulfonyl)-4-dimethylaminopyridinium-1-carboxamide inner salts, depending on the substitution on the arylsulfonamide. Both types of intermediates, gave ester-protected arylsulfonylurea-glucosamines, when treated with 1,3,4,6-tetra-O-acetylglucosamine. Simple methanolysis gave the arylsulfonylurea-glucosamine hybrids as interconverting mixtures of anomers. Both the O-acetyl intermediates and the target arylsulfonylurea-glucosamines inhibited jack-bean urease with IC 50 10–36 μM. This narrow range of values precluded the determination of structure-activity relationships and docking studies suggested several different optimum docking poses for the various analogues. No analogues showed radical-scavenging activity. Several compounds showed modest cytotoxic activity against renal carcinoma cells in the NCI 60-cell-line screen.
ISSN:1054-2523
1554-8120
DOI:10.1007/s00044-024-03208-0