Design of benzimidazoles, benzoxazoles, benzothiazoles and thiazolopyridines as leukotriene A4 hydrolase inhibitors through 3D-QSAR, docking and molecular dynamics

Lorca Marcos; Faúndez Mario; Pessoa-Mahana David C.; Recabarren-Gajardo Gonzalo; Diethelm-Varela Benjamin; Millán Daniela; Celik Ismail; Mellado Marco; Araque Ileana; Mella Jaime; Romero-Parra Javier

doi:10.2298/JSC220427068L

Journal of the Serbian Chemical Society (Jan 2023)

Design of benzimidazoles, benzoxazoles, benzothiazoles and thiazolopyridines as leukotriene A4 hydrolase inhibitors through 3D-QSAR, docking and molecular dynamics

Lorca Marcos,
Faúndez Mario,
Pessoa-Mahana David C.,
Recabarren-Gajardo Gonzalo,
Diethelm-Varela Benjamin,
Millán Daniela,
Celik Ismail,
Mellado Marco,
Araque Ileana,
Mella Jaime,
Romero-Parra Javier

Affiliations

Lorca Marcos: ORCiD; Institute of Chemistry and Biochemistry, Faculty of Science, University of Valparaíso, Valparaíso, Chile
Faúndez Mario: ORCiD; Faculty of Chemistry and Pharmacy, Pontifical Catholic University of Chile, Santiago, Chile
Pessoa-Mahana David C.: ORCiD; Faculty of Chemistry and Pharmacy, Pontifical Catholic University of Chile, Santiago, Chile
Recabarren-Gajardo Gonzalo: ORCiD; Faculty of Chemistry and Pharmacy, Pontifical Catholic University of Chile, Santiago, Chile + Interdisciplinary Center for Neurosciences, Pontifical Catholic University of Chile, Santiago, Chile
Diethelm-Varela Benjamin: ORCiD; Faculty of Chemistry and Pharmacy, Pontifical Catholic University of Chile, Santiago, Chile
Millán Daniela: ORCiD; Integrative Center for Biology and Applied Chemistry, Bernardo O’Higgins University, Santiago, Chile
Celik Ismail: ORCiD; Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Erciyes University, Kayseri, Turkey
Mellado Marco: ORCiD; Instituto de Investigación y Postgrado, Facultad de Ciencias de la Salud, Universidad Central de Chile, Santiago, Chile
Araque Ileana: ORCiD; Institute of Chemistry and Biochemistry, Faculty of Science, University of Valparaíso, Valparaíso, Chile
Mella Jaime: ORCiD; Institute of Chemistry and Biochemistry, Faculty of Science, University of Valparaíso, Valparaíso, Chile + Chilean Pharmacopeia Research Center, University of Valparaíso, Valparaíso, Chile
Romero-Parra Javier: ORCiD; Department of Organic Chemistry and Physical Chemistry, Faculty of Chemistry and Pharmaceutical Sciences, University of Chile, Santiago, Chile

DOI: https://doi.org/10.2298/JSC220427068L
Journal volume & issue: Vol. 88, no. 1
pp. 25 – 39

Abstract

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Human leukotriene A4 hydrolase enzyme (LTA4H) catalyses the biotransformation of the inactive precursor leukotriene A4 (LTA4) to the bioactive Leukotriene B4 (LTB4), which causes many inflammatory responses in the human body. Therefore, the selective inhibition of this enzyme becomes a useful strategy for the treatment of several illnesses such as asthma, allergic rhinitis, cardiovascular diseases, and cancer. Herein we report a 3D-QSAR/ /CoMFA and CoMSIA study on a series of 47 benzimidazoles, benzoxazoles, benzothiazoles and thiazolopyridines reported as potent LTA4H inhibitors. Good statistical parameters were obtained for the best model (q2 = 0.568, r2 ncv = 0.891 and r2 test = 0.851). A new series of 10 compounds capable of inhibiting leukotriene A4 hydrolase with high potency was presented. All designed inhibitors showed low IC50 in nano- and sub-nanomolar ranges, when they were evaluated in 3D-QSAR models. Subsequently, the designed molecules, as well as the least and most active compounds were subjected to docking and molecular dynamics studies into LTA4H. In conclusion, we summarised a thorough structure–activity relationship (SAR) of LTA4H inhibitors of heterocyclic structure. These models can be used for the rational proposal of new inhibitors.

Published in Journal of the Serbian Chemical Society

ISSN: 0352-5139 (Print); 1820-7421 (Online)
Publisher: Serbian Chemical Society
Country of publisher: Serbia
LCC subjects: Science: Chemistry
Website: http://www.shd-pub.org.rs/index.php/JSCS

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