Vasorelaxation Induced by a New Naphthoquinone-Oxime is Mediated by NO-sGC-cGMP Pathway

Bruna P. V. Dantas; Thaís P. Ribeiro; Valéria L. Assis; Fabíola F. Furtado; Kívia S. Assis; Jeziane S. Alves; Tania M.S. Silva; Celso A. Camara; Maria S. França-Silva; Robson C. Veras; Isac A. Medeiros; Jacicarlos L. Alencar; Valdir A. Braga

doi:10.3390/molecules19079773

Molecules (Jul 2014)

Vasorelaxation Induced by a New Naphthoquinone-Oxime is Mediated by NO-sGC-cGMP Pathway

Bruna P. V. Dantas,
Thaís P. Ribeiro,
Valéria L. Assis,
Fabíola F. Furtado,
Kívia S. Assis,
Jeziane S. Alves,
Tania M.S. Silva,
Celso A. Camara,
Maria S. França-Silva,
Robson C. Veras,
Isac A. Medeiros,
Jacicarlos L. Alencar,
Valdir A. Braga

Affiliations

Bruna P. V. Dantas: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Thaís P. Ribeiro: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Valéria L. Assis: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Fabíola F. Furtado: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Kívia S. Assis: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Jeziane S. Alves: Molecular Sciences Department, Federal Rural University of Pernambuco, Recife, PE 52171-900, Brazil
Tania M.S. Silva: Molecular Sciences Department, Federal Rural University of Pernambuco, Recife, PE 52171-900, Brazil
Celso A. Camara: Molecular Sciences Department, Federal Rural University of Pernambuco, Recife, PE 52171-900, Brazil
Maria S. França-Silva: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Robson C. Veras: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Isac A. Medeiros: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Jacicarlos L. Alencar: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil
Valdir A. Braga: Biotechnology Center, Federal University of Paraíba, João Pessoa, PB 58.051-900, Brazil

DOI: https://doi.org/10.3390/molecules19079773
Journal volume & issue: Vol. 19, no. 7
pp. 9773 – 9785

Abstract

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It has been established that oximes cause endothelium-independent relaxation in blood vessels. In the present study, the cardiovascular effects of the new oxime 3-hydroxy-4–(hydroxyimino)-2-(3-methylbut-2-enylnaphtalen-1(4H)-one (Oxime S1) derived from lapachol were evaluated. In normotensive rats, administration of Oxime S1 (10, 15, 20 and 30 mg/Kg, i.v.) produced dose-dependent reduction in blood pressure. In isolated aorta and superior mesenteric artery rings, Oxime S1 induced endothelium-independent and concentration-dependent relaxations (10−8 M to 10−4 M). In addition, Oxime S1-induced vasorelaxations were attenuated by hydroxocobalamin or methylene blue in aorta and by PTIO or ODQ in mesenteric artery rings, suggesting a role for the nitric oxide (NO) pathway. Additionally, Oxime S1 (30 and 100 µM) significantly increased NO concentrations (13.9 ± 1.6 nM and 17.9 ± 4.1 nM, respectively) measured by nitric oxide microsensors. Furthermore, pre-contraction with KCl (80 mM) prevented Oxime S1-derived vasorelaxation in endothelium-denuded aortic rings. Of note, combined treatment with potassium channel inhibitors also reduced Oxime S1-mediated vasorelaxation suggesting a role for potassium channels, more precisely Kir, Kv and KATP channels. We observed the involvement of BKCa channels in Oxime S1-induced relaxation in mesenteric artery rings. In conclusion, these data suggest that the Oxime S1 induces hypotension and vasorelaxation via NO pathway by activating soluble guanylate cyclase (sGC) and K+ channels.

Published in Molecules

ISSN: 1420-3049 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Chemistry: Organic chemistry
Website: http://www.mdpi.com/journal/molecules

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