Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos

Rocha, Patrícia Keytth Lins

Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos

Detalhes bibliográficos
Ano de defesa:	2021
Autor(a) principal:	Rocha, Patrícia Keytth Lins
Orientador(a):	Não Informado pela instituição
Banca de defesa:	Não Informado pela instituição
Tipo de documento:	Tese
Tipo de acesso:	Acesso aberto
Idioma:	por
Instituição de defesa:	Universidade Federal da Paraíba Brasil Farmacologia Programa de Pós-Graduação em Produtos Naturais e Sintéticos Bioativos UFPB
Programa de Pós-Graduação:	Não Informado pela instituição
Departamento:	Não Informado pela instituição
País:	Não Informado pela instituição
Palavras-chave em Português:	Nitratos orgânicos Óxido nítrico Vasorrelaxamento Organic nitrates Nitric oxide Vasorelaxation CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA
Link de acesso:	https://repositorio.ufpb.br/jspui/handle/123456789/21778
Resumo:	Organic nitrates are commonly used in the treatment of cardiovascular disease. In this work, we verified the pharmacological effect of the organic nitrate 4- nitrooxybutyl benzoate (BBN) on the cardiovascular system of rats. The in silico approach was used to predict the biological activities for BBN using the PASS program; while the pharmacokinetic and toxicological properties were analyzed by pkCSM software; and the bioactivation process by molecular docking using Molegro program, which verified the interactions between BBN and the enzymes xanthine oxidoreductase (XOR), aldehyde dehydrogenase (ALDH), cytochrome P450 (CYP450) and glutathione S-transferase (GST). Then, an ex vivo approach was used to verify the effect promoted by BBN in PE (1μM) pre-contracted superior mesenteric artery isolated from rats. In addition, the BBN mechanisms of action and the development of vascular tolerance pre-exposing the mesenteric arteries to a high concentration of BBN (100 μM) were identifying. Among the mechanisms of action, using the inhibitor ODQ (10mM), the participation of the soluble guanylyl cyclase (sGC) enzyme was evaluated; the K+ channels was investigated using the blocker TEA (3mM); also, the inhibition of Ca2+ influx through Cav was analyzed by inductions of contractions with a depolarizing solution KCl (60mM) and with a selective agonist for CaV1, S(-)-Bay K 8644 (200nM). Finally, the in vivo approach was performed to verify the toxicological risk of BBN, administering high doses of the compound (300 or 2000 mg/kg) in rats; and the physiological effect on the cardiovascular system of rats was analyzed by administering intravenous doses of BBN (1; 5; 10; 20 mg/kg) in non-anesthetized rats. As a result of the in silico step, BBN was predicted as a potential vasodilator due to the release of the nitric oxide (NO) molecule from its compound; it was further suggested that BBN had good theoretical oral bioavailability and low toxicity; and interactions between BBN and XOR, ALDH, CYP450 enzymes were identified. In the ex vivo step, the vasorelaxant effect induced by BBN was confirmed. This effect is concentration-dependent and endothelium-independent. Vasorelaxation was significantly attenuated by the soluble sGC inhibitor, suggesting the involvement of the NO-GCs-PKG pathway. It was found that K+ channels were not involved with the BBN-induced effect. However, the inhibition of Ca2+ influx through CaV would participate in the effect promoted by BBN; since BBN was able to inhibit both the contraction mediated by Tyrode's solution with 60 mM KCl and the contraction promoted by S(-)-Bay K 8644. In addition, BBN did not develop vascular tolerance. In the assessment of acute toxicity, no deaths of rats were verified. Acute administration of BBN in rats induced a reduction in mean arterial pressure (MAP) and heart rate (HR) in normotensive and spontaneously hypertensive rats. These results indicate that BBN induces hypotensive and antihypertensive activities in rats.

Metadados do item

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spelling	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratosNitratos orgânicosÓxido nítricoVasorrelaxamentoOrganic nitratesNitric oxideVasorelaxationCNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIAOrganic nitrates are commonly used in the treatment of cardiovascular disease. In this work, we verified the pharmacological effect of the organic nitrate 4- nitrooxybutyl benzoate (BBN) on the cardiovascular system of rats. The in silico approach was used to predict the biological activities for BBN using the PASS program; while the pharmacokinetic and toxicological properties were analyzed by pkCSM software; and the bioactivation process by molecular docking using Molegro program, which verified the interactions between BBN and the enzymes xanthine oxidoreductase (XOR), aldehyde dehydrogenase (ALDH), cytochrome P450 (CYP450) and glutathione S-transferase (GST). Then, an ex vivo approach was used to verify the effect promoted by BBN in PE (1μM) pre-contracted superior mesenteric artery isolated from rats. In addition, the BBN mechanisms of action and the development of vascular tolerance pre-exposing the mesenteric arteries to a high concentration of BBN (100 μM) were identifying. Among the mechanisms of action, using the inhibitor ODQ (10mM), the participation of the soluble guanylyl cyclase (sGC) enzyme was evaluated; the K+ channels was investigated using the blocker TEA (3mM); also, the inhibition of Ca2+ influx through Cav was analyzed by inductions of contractions with a depolarizing solution KCl (60mM) and with a selective agonist for CaV1, S(-)-Bay K 8644 (200nM). Finally, the in vivo approach was performed to verify the toxicological risk of BBN, administering high doses of the compound (300 or 2000 mg/kg) in rats; and the physiological effect on the cardiovascular system of rats was analyzed by administering intravenous doses of BBN (1; 5; 10; 20 mg/kg) in non-anesthetized rats. As a result of the in silico step, BBN was predicted as a potential vasodilator due to the release of the nitric oxide (NO) molecule from its compound; it was further suggested that BBN had good theoretical oral bioavailability and low toxicity; and interactions between BBN and XOR, ALDH, CYP450 enzymes were identified. In the ex vivo step, the vasorelaxant effect induced by BBN was confirmed. This effect is concentration-dependent and endothelium-independent. Vasorelaxation was significantly attenuated by the soluble sGC inhibitor, suggesting the involvement of the NO-GCs-PKG pathway. It was found that K+ channels were not involved with the BBN-induced effect. However, the inhibition of Ca2+ influx through CaV would participate in the effect promoted by BBN; since BBN was able to inhibit both the contraction mediated by Tyrode's solution with 60 mM KCl and the contraction promoted by S(-)-Bay K 8644. In addition, BBN did not develop vascular tolerance. In the assessment of acute toxicity, no deaths of rats were verified. Acute administration of BBN in rats induced a reduction in mean arterial pressure (MAP) and heart rate (HR) in normotensive and spontaneously hypertensive rats. These results indicate that BBN induces hypotensive and antihypertensive activities in rats.Pró-Reitoria de Pós-graduação da UFPB (PRPG/UFPB)Os nitratos orgânicos são comumente utilizados no tratamento de doenças cardiovasculares. Neste trabalho foi verificado o efeito farmacológico do mononitrato orgânico benzoato de 4-nitrooxibutila (BBN) sobre o sistema cardiovascular de ratos. Utilizando abordagem in silico, foram preditas as atividades biológicas para o BBN por meio do programa PASS; as propriedades farmacocinéticas e toxicológicas utilizando o software pkCSM; e o processo de bioativação do BBN pelas enzimas xantina oxirredutase (XOR), aldeído desidrogenase (ALDH), citocromo P450 (CYP450) e glutationa S-transferase (GST) utilizando o programa Molegro. Posteriormente, a abordagem ex vivo foi utilizada para verificar o efeito promovido pelo BBN em artéria mesentérica superior isolada de ratos e pré-contraídas com fenilefrina (PE; 1μM), além de identificar os mecanismos de ação envolvidos na resposta do BBN e avaliar o desenvolvimento da tolerância vascular pré-expondo as artérias mesentéricas a uma alta concentração de BBN (100 μM). Dentre os mecanismos de ação, foi avaliada a participação: da enzima guanilil ciclase soluvel (GCs), utilizando o inibidor ODQ (10mM); dos canais para K+, utilizando o bloqueador TEA (3mM); além da inibição do influxo de Ca2+ pelos Cav, induzindo contrações com uma solução despolarizante KCl (60mM) e com um agonista seletivo para os CaV1, S(-)-Bay K 8644 (200nM). Por último, a abordagem in vivo foi realizada para verificar o risco toxicológico do BBN, administrando altas doses do composto (300 ou 2000 mg/kg) em ratas; e o efeito fisiológico sobre o sistema cardiovascular foi analisado administrando doses intravenosas de BBN (1; 5; 10; 20 mg/kg) em ratos não anestesiados. Como resultados da etapa in silico, o BBN foi predito como um potencial vasodilatador devido à liberação da molécula de óxido nítrico (NO) do seu composto. Pela análise farmacocinética sugeriu-se que o BBN apresenta boa biodisponibilidade oral teórica e baixa toxicidade. O teste de acoragem molecular identificou interações favoráveis entre o BBN com as enzimas XOR, ALDH, CYP450. Na etapa ex vivo foi confirmado o efeito vasorrelaxante induzido pelo BBN. Esse efeito é dependente de concentração e independente dos fatores vasoativos liberados pelo endotélio vascular. O vasorrelaxamento foi significativamente atenuado pelo inibidor da enzima GCs, sugerindo o envolvimento da via NO-GCs-PKG. Foi verificado que os canais de K+ não estão envolvidos com o efeito induzido pelo BBN. Contudo, foi demonstrado que o bloqueio do influxo de Ca2+ pelos CaV participa do efeito promovido pelo BBN, uma vez que o BBN foi capaz de inibir tanto a contração mediada pela solução de Tyrode com 60 mM de KCl quanto a contração promovida pelo S(-)-Bay K 8644. Foi demonstrado ainda que o BBN não desenvolve tolerância vascular. Na avaliação da toxicidade aguda in vivo, não foram observadas mortes das ratas, sugerindo que o BBN apresenta baixa toxicidade. A administração aguda do BBN em ratos induziu redução na pressão arterial média e na frequência cardíaca tanto nos normotensos quanto nos espontaneamente hipertensos. Esses resultados indicam que o BBN induz atividades hipotensoras e anti-hipertensivas em ratos.Universidade Federal da ParaíbaBrasilFarmacologiaPrograma de Pós-Graduação em Produtos Naturais e Sintéticos BioativosUFPBBraga, Valdir de Andradehttp://lattes.cnpq.br/0052252490653096Almeida, Juliana Francohttp://lattes.cnpq.br/8889496706161896Rocha, Patrícia Keytth Lins2021-12-30T16:59:50Z2021-09-272021-12-30T16:59:50Z2021-08-24info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesishttps://repositorio.ufpb.br/jspui/handle/123456789/21778porAttribution-NoDerivs 3.0 Brazilhttp://creativecommons.org/licenses/by-nd/3.0/br/info:eu-repo/semantics/openAccessreponame:Biblioteca Digital de Teses e Dissertações da UFPBinstname:Universidade Federal da Paraíba (UFPB)instacron:UFPB2022-08-09T16:12:53Zoai:repositorio.ufpb.br:123456789/21778Biblioteca Digital de Teses e Dissertaçõeshttps://repositorio.ufpb.br/PUBhttp://tede.biblioteca.ufpb.br:8080/oai/requestdiretoria@ufpb.br\|\| bdtd@biblioteca.ufpb.bropendoar:2022-08-09T16:12:53Biblioteca Digital de Teses e Dissertações da UFPB - Universidade Federal da Paraíba (UFPB)false
dc.title.none.fl_str_mv	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
title	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
spellingShingle	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos Rocha, Patrícia Keytth Lins Nitratos orgânicos Óxido nítrico Vasorrelaxamento Organic nitrates Nitric oxide Vasorelaxation CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA
title_short	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
title_full	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
title_fullStr	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
title_full_unstemmed	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
title_sort	Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos
author	Rocha, Patrícia Keytth Lins
author_facet	Rocha, Patrícia Keytth Lins
author_role	author
dc.contributor.none.fl_str_mv	Braga, Valdir de Andrade http://lattes.cnpq.br/0052252490653096 Almeida, Juliana Franco http://lattes.cnpq.br/8889496706161896
dc.contributor.author.fl_str_mv	Rocha, Patrícia Keytth Lins
dc.subject.por.fl_str_mv	Nitratos orgânicos Óxido nítrico Vasorrelaxamento Organic nitrates Nitric oxide Vasorelaxation CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA
topic	Nitratos orgânicos Óxido nítrico Vasorrelaxamento Organic nitrates Nitric oxide Vasorelaxation CNPQ::CIENCIAS BIOLOGICAS::FARMACOLOGIA
description	Organic nitrates are commonly used in the treatment of cardiovascular disease. In this work, we verified the pharmacological effect of the organic nitrate 4- nitrooxybutyl benzoate (BBN) on the cardiovascular system of rats. The in silico approach was used to predict the biological activities for BBN using the PASS program; while the pharmacokinetic and toxicological properties were analyzed by pkCSM software; and the bioactivation process by molecular docking using Molegro program, which verified the interactions between BBN and the enzymes xanthine oxidoreductase (XOR), aldehyde dehydrogenase (ALDH), cytochrome P450 (CYP450) and glutathione S-transferase (GST). Then, an ex vivo approach was used to verify the effect promoted by BBN in PE (1μM) pre-contracted superior mesenteric artery isolated from rats. In addition, the BBN mechanisms of action and the development of vascular tolerance pre-exposing the mesenteric arteries to a high concentration of BBN (100 μM) were identifying. Among the mechanisms of action, using the inhibitor ODQ (10mM), the participation of the soluble guanylyl cyclase (sGC) enzyme was evaluated; the K+ channels was investigated using the blocker TEA (3mM); also, the inhibition of Ca2+ influx through Cav was analyzed by inductions of contractions with a depolarizing solution KCl (60mM) and with a selective agonist for CaV1, S(-)-Bay K 8644 (200nM). Finally, the in vivo approach was performed to verify the toxicological risk of BBN, administering high doses of the compound (300 or 2000 mg/kg) in rats; and the physiological effect on the cardiovascular system of rats was analyzed by administering intravenous doses of BBN (1; 5; 10; 20 mg/kg) in non-anesthetized rats. As a result of the in silico step, BBN was predicted as a potential vasodilator due to the release of the nitric oxide (NO) molecule from its compound; it was further suggested that BBN had good theoretical oral bioavailability and low toxicity; and interactions between BBN and XOR, ALDH, CYP450 enzymes were identified. In the ex vivo step, the vasorelaxant effect induced by BBN was confirmed. This effect is concentration-dependent and endothelium-independent. Vasorelaxation was significantly attenuated by the soluble sGC inhibitor, suggesting the involvement of the NO-GCs-PKG pathway. It was found that K+ channels were not involved with the BBN-induced effect. However, the inhibition of Ca2+ influx through CaV would participate in the effect promoted by BBN; since BBN was able to inhibit both the contraction mediated by Tyrode's solution with 60 mM KCl and the contraction promoted by S(-)-Bay K 8644. In addition, BBN did not develop vascular tolerance. In the assessment of acute toxicity, no deaths of rats were verified. Acute administration of BBN in rats induced a reduction in mean arterial pressure (MAP) and heart rate (HR) in normotensive and spontaneously hypertensive rats. These results indicate that BBN induces hypotensive and antihypertensive activities in rats.
publishDate	2021
dc.date.none.fl_str_mv	2021-12-30T16:59:50Z 2021-09-27 2021-12-30T16:59:50Z 2021-08-24
dc.type.status.fl_str_mv	info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv	info:eu-repo/semantics/doctoralThesis
format	doctoralThesis
status_str	publishedVersion
dc.identifier.uri.fl_str_mv	https://repositorio.ufpb.br/jspui/handle/123456789/21778
url	https://repositorio.ufpb.br/jspui/handle/123456789/21778
dc.language.iso.fl_str_mv	por
language	por
dc.rights.driver.fl_str_mv	Attribution-NoDerivs 3.0 Brazil http://creativecommons.org/licenses/by-nd/3.0/br/ info:eu-repo/semantics/openAccess
rights_invalid_str_mv	Attribution-NoDerivs 3.0 Brazil http://creativecommons.org/licenses/by-nd/3.0/br/
eu_rights_str_mv	openAccess
dc.publisher.none.fl_str_mv	Universidade Federal da Paraíba Brasil Farmacologia Programa de Pós-Graduação em Produtos Naturais e Sintéticos Bioativos UFPB
publisher.none.fl_str_mv	Universidade Federal da Paraíba Brasil Farmacologia Programa de Pós-Graduação em Produtos Naturais e Sintéticos Bioativos UFPB
dc.source.none.fl_str_mv	reponame:Biblioteca Digital de Teses e Dissertações da UFPB instname:Universidade Federal da Paraíba (UFPB) instacron:UFPB
instname_str	Universidade Federal da Paraíba (UFPB)
instacron_str	UFPB
institution	UFPB
reponame_str	Biblioteca Digital de Teses e Dissertações da UFPB
collection	Biblioteca Digital de Teses e Dissertações da UFPB
repository.name.fl_str_mv	Biblioteca Digital de Teses e Dissertações da UFPB - Universidade Federal da Paraíba (UFPB)
repository.mail.fl_str_mv	diretoria@ufpb.br\|\| bdtd@biblioteca.ufpb.br
_version_	1831315237968543744

Efeito hipotensor e anti-hipertensivo do nitrato orgânico benzoato de 4-nitrooxibutila em ratos

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