Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato
Autor(a) principal: | |
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Data de Publicação: | 2013 |
Tipo de documento: | Dissertação |
Idioma: | por |
Título da fonte: | Repositório Institucional da UFS |
Texto Completo: | https://ri.ufs.br/handle/riufs/3972 |
Resumo: | Linalool is a monoterpene can be biosynthesized by some plants in the racemic form, ( })-linalool, or in the form of enantiomers, (+)-linalool or (-)-linalool. The evaluation the activity of pure isomers has become important in the discovery of new drugs with improved therapeutic potential and a lower rate of adverse effects. So, the objective of the present study was to evaluate the vasorelaxant action induced by the enantiomers, (+) and (-)-linalool in rat superior mesenteric artery, besides seeks to elucidate the mechanisms of action involved in this effect. For both, male Wistar rats (200 . 300 g) were euthanized by exsanguination under anesthesia and superior mesenteric artery was removed. Rings were obtained (1-2 mm) this artery, and were mounted in organ baths containing 10 mL of Tyrode fs solution at 37 C and gassed with carbogen. For isometric tension recordings, each ring was suspended by cotton thread fixed in a force transducer connected to an acquisition system. In rings with functional endothelium pre-contracted with 10 ÊL of phenylephrine, both enantiomers were able to induce significant concentration-dependent vasorelaxation. Such as the effect presented by the (-)-linalool (Emax = 75 } 3%, n = 6) were higher than those for the (+)-linalool (Emax = 41 } 3%, n = 4), sought to evaluate the mechanism of action involved in their action vasorelaxant. In rings without functional endothelium, the vasorelaxation induced by (-)-linalool was significantly attenuated compared to the condition where the rings with functional endothelium were pre-contracted with phenylephrine (Emax = 55 } 1.5%, n = 5). Similar results were obtained after incubation with 10-8 M of atropine, an antagonist of muscarinic receptors (Emax = 50 } 5 %; n = 5); or with 10-4 M of L-NAME, an inhibitor of NO synthesis (Emax = 57 } 5 %; n = 6); or with 30 ÊM of hydroxocobalamin, a NO scavenger (Emax = 45 } 5 %; n = 6). In rings without functional endothelium incubated with 1 mM TEA, a blocker of non-selective K+ channels, the vasorelaxation induced by (-)-linalool had not changed significantly (Emax = 70 } 4 %; n = 4). However, in endothelium-denuded rings pre-contracted with KCl 80 mM, the oil-induced relaxation was significantly higher than that obtained without functional endothelium in rings pre-contracted with phenylephrine (Emax = 92 } 2 %; n = 5). In addition, isolated concentrations of (-)-linalool significantly reduced the contractions induced by CaCl2 (10-6 . 10-2 M) or by Na3VO4 (10-5 . 3 x 10-2 M), a non-selective inhibitor of protein tyrosine phosphatases. These results suggest that the effects induced by linalool occur mainly by the action of one of its isomers, the (-)-linalool. This isomer produces an effect vasorelaxant in rat superior mesenteric artery which is in part, dependent on the endothelium which is given by the activation of muscarinic receptors and the NO release. Furthermore, the endothelium-independent vasorelaxation is due to inhibition of calcium channel voltage-sensitive and involves the sensitization of the contractile machinery in vascular smooth muscle. |
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Cunha, Patrícia Santoshttp://lattes.cnpq.br/9692770802439503Santos, Márcio Roberto Viana doshttp://lattes.cnpq.br/28479899556487962017-09-26T12:31:14Z2017-09-26T12:31:14Z2013-08-02https://ri.ufs.br/handle/riufs/3972Linalool is a monoterpene can be biosynthesized by some plants in the racemic form, ( })-linalool, or in the form of enantiomers, (+)-linalool or (-)-linalool. The evaluation the activity of pure isomers has become important in the discovery of new drugs with improved therapeutic potential and a lower rate of adverse effects. So, the objective of the present study was to evaluate the vasorelaxant action induced by the enantiomers, (+) and (-)-linalool in rat superior mesenteric artery, besides seeks to elucidate the mechanisms of action involved in this effect. For both, male Wistar rats (200 . 300 g) were euthanized by exsanguination under anesthesia and superior mesenteric artery was removed. Rings were obtained (1-2 mm) this artery, and were mounted in organ baths containing 10 mL of Tyrode fs solution at 37 C and gassed with carbogen. For isometric tension recordings, each ring was suspended by cotton thread fixed in a force transducer connected to an acquisition system. In rings with functional endothelium pre-contracted with 10 ÊL of phenylephrine, both enantiomers were able to induce significant concentration-dependent vasorelaxation. Such as the effect presented by the (-)-linalool (Emax = 75 } 3%, n = 6) were higher than those for the (+)-linalool (Emax = 41 } 3%, n = 4), sought to evaluate the mechanism of action involved in their action vasorelaxant. In rings without functional endothelium, the vasorelaxation induced by (-)-linalool was significantly attenuated compared to the condition where the rings with functional endothelium were pre-contracted with phenylephrine (Emax = 55 } 1.5%, n = 5). Similar results were obtained after incubation with 10-8 M of atropine, an antagonist of muscarinic receptors (Emax = 50 } 5 %; n = 5); or with 10-4 M of L-NAME, an inhibitor of NO synthesis (Emax = 57 } 5 %; n = 6); or with 30 ÊM of hydroxocobalamin, a NO scavenger (Emax = 45 } 5 %; n = 6). In rings without functional endothelium incubated with 1 mM TEA, a blocker of non-selective K+ channels, the vasorelaxation induced by (-)-linalool had not changed significantly (Emax = 70 } 4 %; n = 4). However, in endothelium-denuded rings pre-contracted with KCl 80 mM, the oil-induced relaxation was significantly higher than that obtained without functional endothelium in rings pre-contracted with phenylephrine (Emax = 92 } 2 %; n = 5). In addition, isolated concentrations of (-)-linalool significantly reduced the contractions induced by CaCl2 (10-6 . 10-2 M) or by Na3VO4 (10-5 . 3 x 10-2 M), a non-selective inhibitor of protein tyrosine phosphatases. These results suggest that the effects induced by linalool occur mainly by the action of one of its isomers, the (-)-linalool. This isomer produces an effect vasorelaxant in rat superior mesenteric artery which is in part, dependent on the endothelium which is given by the activation of muscarinic receptors and the NO release. Furthermore, the endothelium-independent vasorelaxation is due to inhibition of calcium channel voltage-sensitive and involves the sensitization of the contractile machinery in vascular smooth muscle.Linalol e um monoterpeno que pode ser biossintetizado por algumas plantas na forma racemica, ( })-linalol, ou na forma de enantiomeros, (+)-linalol ou (-)-linalol. A avaliacao da atividade dos isomeros puros tem tornado-se importante para a descoberta de novas drogas com melhor potencial terapeutico e menor indice de efeitos colaterais. Assim, o objetivo do presente estudo foi avaliar a acao vasorelaxante induzida pelos enantiomeros, (+) e (-)-linalol em arteria mesenterica superior de rato, alem de buscar elucidar os mecanismos envolvidos neste efeito. Para tanto, ratos Wistar machos (200 . 300 g) foram sacrificados por dessangramento sob anestesia e a arteria mesenterica superior foi removida. Desta arteria foram obtidos aneis (1-2 mm) que foram mantidos em cubas para orgao isolado contendo 10 mL de solucao nutritiva de Tyrode a 37 oC e gaseificada com carbogenio. Para o registro das contracoes isometricas, cada anel foi suspenso por linha de algodao fixada a um transdutor de forca conectado a um sistema de aquisicao de dados. Em aneis com endotelio funcional pre-contraidos com 10 ÊM fenilefrina, ambos enantiomeros foram capazes de induzir vasorelaxamento significativo dependente da concentracao. Como o efeito apresentado pelo (-)-linalol (Emax = 75 } 3 %; n = 6) foi maior que aquele apresentado pelo (+)-linalol (Emax = 41 } 3 %; n = 4), buscou-se avaliar o mecanismo de acao envolvido em sua acao vasorelaxante. Em aneis sem endotelio funcional, o vasorelaxamento induzido pelo (-)-linalol foi significativamente atenuado em relacao a condicao onde os aneis com endotelio funcional foram pre-contraidos com fenilefrina (Emax = 55 } 1,5 %; n = 5). Resultados semelhantes foram obtidos apos incubacao com 10-8 M de atropina, um antagonista de receptores muscarinicos (Emax = 50 } 5 %; n = 5); ou 10-4 M de L-NAME, um inibidor da sintese de NO (Emax = 57 } 5 %; n = 6); ou 30 ÊM de hidroxocobalamina, um sequestrador de NO (Emax = 45 } 5 %; n = 6). Em aneis sem endotelio funcional pre-incubados com 1 mM de TEA, um bloqueador nao seletivo de canais para K+, o vasorelaxamento induzido pelo (-)-linalol nao foi alterado significativamente (Emax = 70 } 4 %; n = 4). Porem, em aneis sem endotelio funcional pre-contraidos com KCl 80 mM, o vasorelaxamento induzido pelo oleo foi significativamente maior que aquele obtido em aneis sem endotelio funcional pre-contraidos com fenilefrina (Emax = 92 } 2 %; n = 5). Alem disso, concentracoes isoladas de (-)-linalol foram capazes de antagonizar contracoes induzidas por CaCl2 (10-6 . 10-2 M) e Na3VO4 (10-5 . 3 x 10-2 M), um inibidor nao-seletivo de proteinas tirosina-fosfatases. Estes resultados sugerem que os efeitos induzidos pelo linalol ocorrem, principalmente, pela acao de um de seus isomeros, o (-)-linalol. Este isomero produz um efeito vasorelaxante em arteria mesenterica superior de rato que e em parte, dependente do endotelio, o qual se da pela ativacao de receptores muscarinicos e pela liberacao de NO. Alem disso, o vasorelaxamento independente do endotelio e decorrente da inibicao dos canais para calcio sensiveis a voltagem e envolve a sensibilizacao da maquinaria contratil na musculatura lisa vascular.application/pdfporVasodilatadoresArtéria mesentéricaLinalolSistema cardiovascularEnantiômerosVasos sanguineosIsomerismoVasorelaxamentoCardiovascular systemEnantiomersLinaloolMesenteric arteryVasodilatorsCNPQ::CIENCIAS BIOLOGICAS::FISIOLOGIAEfeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de ratoinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisPós-Graduação em Ciências Fisiológicasinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFSinstname:Universidade Federal de Sergipe (UFS)instacron:UFSTEXTPATRICIA_SANTOS_CUNHA.pdf.txtPATRICIA_SANTOS_CUNHA.pdf.txtExtracted texttext/plain117027https://ri.ufs.br/jspui/bitstream/riufs/3972/2/PATRICIA_SANTOS_CUNHA.pdf.txtb02e136a0f5e7c02d4812c68c6c2ce54MD52THUMBNAILPATRICIA_SANTOS_CUNHA.pdf.jpgPATRICIA_SANTOS_CUNHA.pdf.jpgGenerated Thumbnailimage/jpeg1270https://ri.ufs.br/jspui/bitstream/riufs/3972/3/PATRICIA_SANTOS_CUNHA.pdf.jpg7ae4f7312e7e7e3c7dfb320dcc171a10MD53ORIGINALPATRICIA_SANTOS_CUNHA.pdfapplication/pdf968672https://ri.ufs.br/jspui/bitstream/riufs/3972/1/PATRICIA_SANTOS_CUNHA.pdf7c2d877066cb8394e715b4ce1f9c1de1MD51riufs/39722017-11-24 21:46:12.24oai:ufs.br:riufs/3972Repositório InstitucionalPUBhttps://ri.ufs.br/oai/requestrepositorio@academico.ufs.bropendoar:2017-11-25T00:46:12Repositório Institucional da UFS - Universidade Federal de Sergipe (UFS)false |
dc.title.por.fl_str_mv |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
title |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
spellingShingle |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato Cunha, Patrícia Santos Vasodilatadores Artéria mesentérica Linalol Sistema cardiovascular Enantiômeros Vasos sanguineos Isomerismo Vasorelaxamento Cardiovascular system Enantiomers Linalool Mesenteric artery Vasodilators CNPQ::CIENCIAS BIOLOGICAS::FISIOLOGIA |
title_short |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
title_full |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
title_fullStr |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
title_full_unstemmed |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
title_sort |
Efeito vasorelaxante dos isômeros (+) e (-)-linalol em artéria mesentérica de rato |
author |
Cunha, Patrícia Santos |
author_facet |
Cunha, Patrícia Santos |
author_role |
author |
dc.contributor.author.fl_str_mv |
Cunha, Patrícia Santos |
dc.contributor.advisor1Lattes.fl_str_mv |
http://lattes.cnpq.br/9692770802439503 |
dc.contributor.advisor1.fl_str_mv |
Santos, Márcio Roberto Viana dos |
dc.contributor.authorLattes.fl_str_mv |
http://lattes.cnpq.br/2847989955648796 |
contributor_str_mv |
Santos, Márcio Roberto Viana dos |
dc.subject.por.fl_str_mv |
Vasodilatadores Artéria mesentérica Linalol Sistema cardiovascular Enantiômeros Vasos sanguineos Isomerismo Vasorelaxamento |
topic |
Vasodilatadores Artéria mesentérica Linalol Sistema cardiovascular Enantiômeros Vasos sanguineos Isomerismo Vasorelaxamento Cardiovascular system Enantiomers Linalool Mesenteric artery Vasodilators CNPQ::CIENCIAS BIOLOGICAS::FISIOLOGIA |
dc.subject.eng.fl_str_mv |
Cardiovascular system Enantiomers Linalool Mesenteric artery Vasodilators |
dc.subject.cnpq.fl_str_mv |
CNPQ::CIENCIAS BIOLOGICAS::FISIOLOGIA |
description |
Linalool is a monoterpene can be biosynthesized by some plants in the racemic form, ( })-linalool, or in the form of enantiomers, (+)-linalool or (-)-linalool. The evaluation the activity of pure isomers has become important in the discovery of new drugs with improved therapeutic potential and a lower rate of adverse effects. So, the objective of the present study was to evaluate the vasorelaxant action induced by the enantiomers, (+) and (-)-linalool in rat superior mesenteric artery, besides seeks to elucidate the mechanisms of action involved in this effect. For both, male Wistar rats (200 . 300 g) were euthanized by exsanguination under anesthesia and superior mesenteric artery was removed. Rings were obtained (1-2 mm) this artery, and were mounted in organ baths containing 10 mL of Tyrode fs solution at 37 C and gassed with carbogen. For isometric tension recordings, each ring was suspended by cotton thread fixed in a force transducer connected to an acquisition system. In rings with functional endothelium pre-contracted with 10 ÊL of phenylephrine, both enantiomers were able to induce significant concentration-dependent vasorelaxation. Such as the effect presented by the (-)-linalool (Emax = 75 } 3%, n = 6) were higher than those for the (+)-linalool (Emax = 41 } 3%, n = 4), sought to evaluate the mechanism of action involved in their action vasorelaxant. In rings without functional endothelium, the vasorelaxation induced by (-)-linalool was significantly attenuated compared to the condition where the rings with functional endothelium were pre-contracted with phenylephrine (Emax = 55 } 1.5%, n = 5). Similar results were obtained after incubation with 10-8 M of atropine, an antagonist of muscarinic receptors (Emax = 50 } 5 %; n = 5); or with 10-4 M of L-NAME, an inhibitor of NO synthesis (Emax = 57 } 5 %; n = 6); or with 30 ÊM of hydroxocobalamin, a NO scavenger (Emax = 45 } 5 %; n = 6). In rings without functional endothelium incubated with 1 mM TEA, a blocker of non-selective K+ channels, the vasorelaxation induced by (-)-linalool had not changed significantly (Emax = 70 } 4 %; n = 4). However, in endothelium-denuded rings pre-contracted with KCl 80 mM, the oil-induced relaxation was significantly higher than that obtained without functional endothelium in rings pre-contracted with phenylephrine (Emax = 92 } 2 %; n = 5). In addition, isolated concentrations of (-)-linalool significantly reduced the contractions induced by CaCl2 (10-6 . 10-2 M) or by Na3VO4 (10-5 . 3 x 10-2 M), a non-selective inhibitor of protein tyrosine phosphatases. These results suggest that the effects induced by linalool occur mainly by the action of one of its isomers, the (-)-linalool. This isomer produces an effect vasorelaxant in rat superior mesenteric artery which is in part, dependent on the endothelium which is given by the activation of muscarinic receptors and the NO release. Furthermore, the endothelium-independent vasorelaxation is due to inhibition of calcium channel voltage-sensitive and involves the sensitization of the contractile machinery in vascular smooth muscle. |
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2013 |
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2013-08-02 |
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