| Literature DB >> 25712353 |
Nayara Cristina Fonseca1, Luana Faria da Cruz2, Filipe da Silva Villela2, Glaécia Aparecida do Nascimento Pereira3, Jair Lage de Siqueira-Neto4, Danielle Kellar5, Brian M Suzuki5, Debalina Ray5, Thiago Belarmino de Souza1, Ricardo José Alves1, Policarpo Ademar Sales Júnior6, Alvaro José Romanha7, Silvane Maria Fonseca Murta6, James H McKerrow4, Conor R Caffrey5, Renata Barbosa de Oliveira1, Rafaela Salgado Ferreira8.
Abstract
The pressing need for better drugs against Chagas disease, African sleeping sickness, and schistosomiasis motivates the search for inhibitors of cruzain, rhodesain, and Schistosoma mansoni CB1 (SmCB1), the major cysteine proteases from Trypanosoma cruzi, Trypanosoma brucei, and S. mansoni, respectively. Thiosemicarbazones and heterocyclic analogues have been shown to be both antitrypanocidal and inhibitory against parasite cysteine proteases. A series of compounds was synthesized and evaluated against cruzain, rhodesain, and SmCB1 through biochemical assays to determine their potency and structure-activity relationships (SAR). This approach led to the discovery of 6 rhodesain, 4 cruzain, and 5 SmCB1 inhibitors with 50% inhibitory concentrations (IC50s) of ≤ 10 μM. Among the compounds tested, the thiosemicarbazone derivative of peracetylated galactoside (compound 4i) was discovered to be a potent rhodesain inhibitor (IC50 = 1.2 ± 1.0 μM). The impact of a range of modifications was determined; removal of thiosemicarbazone or its replacement by semicarbazone resulted in virtually inactive compounds, and modifications in the sugar also diminished potency. Compounds were also evaluated in vitro against the parasites T. cruzi, T. brucei, and S. mansoni, revealing active compounds among this series.Entities:
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Year: 2015 PMID: 25712353 PMCID: PMC4394791 DOI: 10.1128/AAC.04601-14
Source DB: PubMed Journal: Antimicrob Agents Chemother ISSN: 0066-4804 Impact factor: 5.191