2-(pyridin-4yl)benzothiazole and its benzimidazole-analogue: biophysical and in silico studies on their interaction with urease and in vitro anti-Helicobacter pylori activities

Camila P. Pereira; Luzia Valentina Modolo; Josué Carinhanha Caldas Santos; Ângelo de Fátima; Ana Carolina Fradique de Lyra; Breno Germano de Freitas Oliveira; Igor José dos Santos Nascimento; Edeildo Ferreira da Silva-Júnior; Thiago Mendonça de Aquino; Francesca Sisto; Isis Martins Figueiredo; Felipe Terra Martins

Use este identificador para citar o ir al link de este elemento: http://hdl.handle.net/1843/78030

Tipo:	Artigo de Periódico
Título:	2-(pyridin-4yl)benzothiazole and its benzimidazole-analogue: biophysical and in silico studies on their interaction with urease and in vitro anti-Helicobacter pylori activities
Autor(es):	Camila P. Pereira Luzia Valentina Modolo Josué Carinhanha Caldas Santos Ângelo de Fátima Ana Carolina Fradique de Lyra Breno Germano de Freitas Oliveira Igor José dos Santos Nascimento Edeildo Ferreira da Silva-Júnior Thiago Mendonça de Aquino Francesca Sisto Isis Martins Figueiredo Felipe Terra Martins
Resumen:	In this study, the interaction between benzothiazole (BTA, concentration of a drug required for 50% inhibition in vitro (IC 50) = 0.77 mM) and benzimidazole (BIA, IC 50 = 2.14 mM) with urease was quantitatively assessed, using UV-Vis, molecular fluorescence, and circular dichroism. The results showed that both compounds interact with urease by a static fluorescence quenching mechanism with a non-fluorescent complex formation. The main forces responsible for stabilizing the supramolecular complex between BTA and urease were hydrophobic while, for BIA, van der Waals interactions and hydrogen bonds were the main ones. Urease conformation changes due to the interaction process were analyzed by circular dichroism and synchronous fluorescence. Besides, a competitive assay with substrate and inhibitors was used to evaluate the preferential urease site of interaction with BTA and BIA. Our experimental and theoretical studies supported that both, BTA and BIA, are mixed-inhibitors of ureases with a slight preference to the active site of such enzymes. Finally, both BTA and BIA showed to possess anti-Helicobacter pylori (one reference strain and six clinical isolates) activity, presenting minimal inhibitory concentration (MIC) values ranging from 38-150 and 20-164 μM, respectively. The urease inhibitors omeprazole and hydroxyurea showed MIC values in the range of 46-185 μM and 1683-> 3366 μM, respectively.
Asunto:	Urease - Inibidores Benzimidazois Helicobacter pylori Enzimas
Idioma:	eng
País:	Brasil
Editor:	Universidade Federal de Minas Gerais
Sigla da Institución:	UFMG
Departamento:	ICB - DEPARTAMENTO DE BOTÂNICA ICX - DEPARTAMENTO DE QUÍMICA
Tipo de acceso:	Acesso Aberto
Identificador DOI:	https://dx.doi.org/10.21577/0103-5053.20220020
URI:	http://hdl.handle.net/1843/78030
Fecha del documento:	2022
metadata.dc.url.externa:	https://jbcs.sbq.org.br/default.asp?ed=330
metadata.dc.relation.ispartof:	Journal of the Brazilian Chemical Society
Aparece en las colecciones:	Artigo de Periódico

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