Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio

Detalhes bibliográficos
Autor(a) principal: Castardeli, Carmen
Data de Publicação: 2016
Tipo de documento: Dissertação
Idioma: por
Título da fonte: Repositório Institucional da Universidade Federal do Espírito Santo (riUfes)
Texto Completo: http://repositorio.ufes.br/handle/10/7889
Resumo: Diminazene aceturate (DIZE) is used with an antitrypanosomal action for veterinary use which is also able to increase the catalytic efficiency of ACE-2. Thus the objective of our work was to investigate the effects of DIZE on the postinfarction cardiac remodeling process. Besides that, data with DIZE treatment were compared to those obtained in the same experimental model submitted to Losartan (Los). Rats Male Wistar were submitted to a surgical procedure to produce permanent occlusion of the left coronary artery to produce MI, the control animals underwent the same surgical procedure but without arterial occlusion. After surgery the animals were divided into five groups: (1) Control Rats + Placebo (Pla-Con, n = 8); (2) Controls Rats + DIZE (Con-DIZE; n = 6); (3) Infarcted Rats + Placebo (Pla-IM, n = 7); (4) Infarcted Rats + DIZE (IM-SAY; n = 6); (5) Infarcted Rats + Losartan (MI-Los; n = 7) were administered daily subcutaneous injection of 15 mg / kg (DIZE and / or LOS) and Placebo (0.9% NaCl) for 28 days. After 28 days the animals were anesthetized to record the intracardiac hemodynamic variables. After recording hemodynamic variables, the cardiac beats were stopped diastole with an intravenous injection of KCl (1 M). A double lumen catheter was inserted into the left ventricular cavity to obtain the record of the pressurevolume curve. Hearts were fixed in formalin and processed to histological analysis of myocyte hypertrophy and collagen content. The group IM-Pla presented a significant increase in the left ventricular end diastolic pressure (LVEDP = 26±3,3 mmHg) and also a significant reduction of +dP/dt (3014 ± 161 mmHg/s), -dP/dt ( -2333±91 mmHg/s) and systolic blood pressure (SBP = 101±3 mmHg), as compared with the groups treated with DIZE (LVEDP = 15±1,6 mmHg/s; +dP/dt 3884±104 mmHg/s; -dPdt = -2798±120 mmHg/s and SVE = 110±0,7 mmHg) or Los (LVEDP = 16±2,9 mmHg; +dP/dt: 4146±131 mmHg/s; -dPdt = -2823±136 mmHg/s; SBP = 111±3,5 mmHg). The right ventricle hemodynamic revealed an increase in systolic pressure in the IM-Pla group (40±0,6 mmHg) with a small decrease in the IM group under DIZE (37±2 mmHg). The IM-DIZE (0,33±0,03 mmHg/mL e 0,64±0,01 mmHg/mL) and IM-Los (0,36±0,03 mmHg/mL e 0,65±0,04 mmHg/mL) groups showed less left ventricular dilatation and stiffness as compared with the infarcted group under Pla (0,39±0,03 mmHg/mL e 0,78±0,02 mmHg/mL). The volumetric fraction of collagen in the surviving left ventricular myocardium increased, was partially prevented by DIZE or Los treatment. The postinfarction hypertrophy of cardiomyocytes, however, remained unaffected by DIZE treatment. As expected, treatment with losartan attenuated the hypertrophic growth in the left ventricle. In conclusion, our study showed that DIZE was effective to partially prevent the hemodynamic changes induced by infarction in rats similarly to the observation in infracted rats treated with Los. The two drugs also prevented the increase in the collagen deposition in the surviving left ventricular myocardium. In relation to the hypertrophic of cardiomyocytes, however, only Los showed a preventive effect.
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spelling Mill, José GeraldoCastardeli, CarmenLeopoldo, André SoaresBaldo, Marcelo Perim2018-08-01T22:58:25Z2018-08-012018-08-01T22:58:25Z2016-09-29Diminazene aceturate (DIZE) is used with an antitrypanosomal action for veterinary use which is also able to increase the catalytic efficiency of ACE-2. Thus the objective of our work was to investigate the effects of DIZE on the postinfarction cardiac remodeling process. Besides that, data with DIZE treatment were compared to those obtained in the same experimental model submitted to Losartan (Los). Rats Male Wistar were submitted to a surgical procedure to produce permanent occlusion of the left coronary artery to produce MI, the control animals underwent the same surgical procedure but without arterial occlusion. After surgery the animals were divided into five groups: (1) Control Rats + Placebo (Pla-Con, n = 8); (2) Controls Rats + DIZE (Con-DIZE; n = 6); (3) Infarcted Rats + Placebo (Pla-IM, n = 7); (4) Infarcted Rats + DIZE (IM-SAY; n = 6); (5) Infarcted Rats + Losartan (MI-Los; n = 7) were administered daily subcutaneous injection of 15 mg / kg (DIZE and / or LOS) and Placebo (0.9% NaCl) for 28 days. After 28 days the animals were anesthetized to record the intracardiac hemodynamic variables. After recording hemodynamic variables, the cardiac beats were stopped diastole with an intravenous injection of KCl (1 M). A double lumen catheter was inserted into the left ventricular cavity to obtain the record of the pressurevolume curve. Hearts were fixed in formalin and processed to histological analysis of myocyte hypertrophy and collagen content. The group IM-Pla presented a significant increase in the left ventricular end diastolic pressure (LVEDP = 26±3,3 mmHg) and also a significant reduction of +dP/dt (3014 ± 161 mmHg/s), -dP/dt ( -2333±91 mmHg/s) and systolic blood pressure (SBP = 101±3 mmHg), as compared with the groups treated with DIZE (LVEDP = 15±1,6 mmHg/s; +dP/dt 3884±104 mmHg/s; -dPdt = -2798±120 mmHg/s and SVE = 110±0,7 mmHg) or Los (LVEDP = 16±2,9 mmHg; +dP/dt: 4146±131 mmHg/s; -dPdt = -2823±136 mmHg/s; SBP = 111±3,5 mmHg). The right ventricle hemodynamic revealed an increase in systolic pressure in the IM-Pla group (40±0,6 mmHg) with a small decrease in the IM group under DIZE (37±2 mmHg). The IM-DIZE (0,33±0,03 mmHg/mL e 0,64±0,01 mmHg/mL) and IM-Los (0,36±0,03 mmHg/mL e 0,65±0,04 mmHg/mL) groups showed less left ventricular dilatation and stiffness as compared with the infarcted group under Pla (0,39±0,03 mmHg/mL e 0,78±0,02 mmHg/mL). The volumetric fraction of collagen in the surviving left ventricular myocardium increased, was partially prevented by DIZE or Los treatment. The postinfarction hypertrophy of cardiomyocytes, however, remained unaffected by DIZE treatment. As expected, treatment with losartan attenuated the hypertrophic growth in the left ventricle. In conclusion, our study showed that DIZE was effective to partially prevent the hemodynamic changes induced by infarction in rats similarly to the observation in infracted rats treated with Los. The two drugs also prevented the increase in the collagen deposition in the surviving left ventricular myocardium. In relation to the hypertrophic of cardiomyocytes, however, only Los showed a preventive effect.O Aceturato de Diminazeno (DIZE) é utilizado como medicamento anti- trypanosomal de uso veterinário que é capaz de aumentar a velocidade catalítica da enzima conversora de angiotensina- 2 (ECA-2). Portanto, o objetivo do nosso trabalho foi investigar os efeitos do tratamento com DIZE no remodelamento cardíaco após infarto agudo do miocárdio (IAM). Além disso, a proposta foi comparar os dados do tratamento com DIZE com modelo experimental tratado com Losartan (Los). Ratos Wistar Macho foram submetidos ao procedimento cirúrgico de oclusão permanente da artéria coronária esquerda para produzir IAM, os animais controles foram submetidos ao mesmo procedimento cirúrgico, porém sem a oclusão arterial. Após a cirurgia os animais foram distribuídos em cinco grupos: (1) Ratos Controles + Placebo (Con-Pla; n= 8); (2) Ratos Controles + DIZE (Con-DIZE; n= 6); (3) Ratos Infartados + Placebo (IM-Pla; n= 7); (4) Ratos Infartados + DIZE (IM-DIZE; n= 6); (5) Ratos Infartados + Losartan (IM-Los; n= 7), foram administrados diariamente injeção subcutânea de 15 mg/kg (DIZE e/ou Los) e placebo (NaCl 0.9%), durante 28 dias. Após 28 dias os animais foram anestesiados para obter as variáveis hemodinâmicas intracardíaca. Após registro hemodinâmico o coração foi parado em diástole com uma injeção intravenosa de KC1 (1M). Um cateter de duplo lúmen foi inserido dentro da cavidade do ventrículo esquerdo (VE) para obter os dados da curva pressão volume. Os Corações foram fixados em paraformol e processados para análise histológica de hipertrofia dos miócitos e conteúdo de colágeno. O grupo IM-Pla apresentou aumento significativo da pressão diastólica final do ventrículo esquerdo (26±3,3 mmHg) e redução na dp/dt+ (3014 ± 161 mmHg/s) e dpdt- ( -2333±91 mmHg/s) e pressão sistólica do VE (101±3,1 mmHg), quando comparados com os grupos tratados com DIZE (PDFVE: 15±1,6 mmHg/s; dp/dt+ 3884±104 mmHg/s; dpdt-: -2798±120 e PSVE: 110±0,7 mmHg) e IM-Los (PDFVE: 16±2,9; dp/dt+: 4146±131 mmHg/s; dpdt-: 2823±136 mmHg/s e PSVE: 111±3,5 mmHg). A hemodinâmica do ventrículo direito (VD) mostrou aumento de pressão do VD no grupo IM-Pla (40±0,6 mmHg) e redução da pressão no grupo IM-DIZE (37±2 mmHg). Os grupos de IM-DIZE (0,33±0,03 mmHg/mL e 0,64±0,01 mmHg/mL) e IM-Los (0,36±0,03 mmHg/mL e 0,65±0,04 mmHg/mL) apresentaram menor dilatação e rigidez no ventrículo esquerdo, quando comparados com com o grupo infartados sobre Pla (0,39±0,03 mmHg/mL e 0,78±0,02 mmHg/mL). O aumento da fração volumétrica de colágeno no VE foi parcialmente prevenido pelo tratamendo com DIZE ou Los. A hipertrofia dos miocitos pós-infarto permaneceu inalterado pelo tratamento com DIZE. Como esperado o tratamento com losartan atenuou o crescimento hipertrófico no ventriclo esquerdo quando comparado aos grupos controles. Em conclusão, nosso estudo apresentou que o DIZE foi parcialmente eficaz para prevenção de mudanças hemodinâmicas induzidas por infarto em ratos semelhante à observação em ratos infartados tratados com Los. As duas drogas também previnem o aumento da deposição de colágeno no miocárdio do ventrículo esquerdo. Em relação a hipertrofia dos miocitos, porém, apenas Los apresentou um efeito preventivo.Texthttp://repositorio.ufes.br/handle/10/7889porUniversidade Federal do Espírito SantoMestrado em Ciências FisiológicasPrograma de Pós-Graduação em Ciências FisiológicasUFESBRCentro de Ciências da SaúdeMyocardial infarctionACE-2DiminazeneHeart failureInfarto do miocárdioECA-2DiminazenoLosartanInsuficiência cardíacaFisiologia612Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdioinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da Universidade Federal do Espírito Santo (riUfes)instname:Universidade Federal do Espírito Santo (UFES)instacron:UFESORIGINALtese_10355_Dissertação Carmen Castardeli.pdfapplication/pdf1558080http://repositorio.ufes.br/bitstreams/98f4bbb8-7377-47e8-b299-8d978c33434f/download7f5f29f1bbfff9d6af681515b8add865MD5110/78892024-07-16 17:09:16.033oai:repositorio.ufes.br:10/7889http://repositorio.ufes.brRepositório InstitucionalPUBhttp://repositorio.ufes.br/oai/requestopendoar:21082024-10-15T17:56:18.853231Repositório Institucional da Universidade Federal do Espírito Santo (riUfes) - Universidade Federal do Espírito Santo (UFES)false
dc.title.none.fl_str_mv Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
title Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
spellingShingle Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
Castardeli, Carmen
Myocardial infarction
ACE-2
Diminazene
Heart failure
Infarto do miocárdio
ECA-2
Diminazeno
Losartan
Insuficiência cardíaca
Fisiologia
612
title_short Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
title_full Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
title_fullStr Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
title_full_unstemmed Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
title_sort Efeito do diminazeno, um ativador da ECA-2, no remodelamento cardíaco de ratos submetidos ao infarto do miocárdio
author Castardeli, Carmen
author_facet Castardeli, Carmen
author_role author
dc.contributor.advisor1.fl_str_mv Mill, José Geraldo
dc.contributor.author.fl_str_mv Castardeli, Carmen
dc.contributor.referee1.fl_str_mv Leopoldo, André Soares
dc.contributor.referee2.fl_str_mv Baldo, Marcelo Perim
contributor_str_mv Mill, José Geraldo
Leopoldo, André Soares
Baldo, Marcelo Perim
dc.subject.eng.fl_str_mv Myocardial infarction
ACE-2
Diminazene
Heart failure
topic Myocardial infarction
ACE-2
Diminazene
Heart failure
Infarto do miocárdio
ECA-2
Diminazeno
Losartan
Insuficiência cardíaca
Fisiologia
612
dc.subject.por.fl_str_mv Infarto do miocárdio
ECA-2
Diminazeno
Losartan
Insuficiência cardíaca
dc.subject.cnpq.fl_str_mv Fisiologia
dc.subject.udc.none.fl_str_mv 612
description Diminazene aceturate (DIZE) is used with an antitrypanosomal action for veterinary use which is also able to increase the catalytic efficiency of ACE-2. Thus the objective of our work was to investigate the effects of DIZE on the postinfarction cardiac remodeling process. Besides that, data with DIZE treatment were compared to those obtained in the same experimental model submitted to Losartan (Los). Rats Male Wistar were submitted to a surgical procedure to produce permanent occlusion of the left coronary artery to produce MI, the control animals underwent the same surgical procedure but without arterial occlusion. After surgery the animals were divided into five groups: (1) Control Rats + Placebo (Pla-Con, n = 8); (2) Controls Rats + DIZE (Con-DIZE; n = 6); (3) Infarcted Rats + Placebo (Pla-IM, n = 7); (4) Infarcted Rats + DIZE (IM-SAY; n = 6); (5) Infarcted Rats + Losartan (MI-Los; n = 7) were administered daily subcutaneous injection of 15 mg / kg (DIZE and / or LOS) and Placebo (0.9% NaCl) for 28 days. After 28 days the animals were anesthetized to record the intracardiac hemodynamic variables. After recording hemodynamic variables, the cardiac beats were stopped diastole with an intravenous injection of KCl (1 M). A double lumen catheter was inserted into the left ventricular cavity to obtain the record of the pressurevolume curve. Hearts were fixed in formalin and processed to histological analysis of myocyte hypertrophy and collagen content. The group IM-Pla presented a significant increase in the left ventricular end diastolic pressure (LVEDP = 26±3,3 mmHg) and also a significant reduction of +dP/dt (3014 ± 161 mmHg/s), -dP/dt ( -2333±91 mmHg/s) and systolic blood pressure (SBP = 101±3 mmHg), as compared with the groups treated with DIZE (LVEDP = 15±1,6 mmHg/s; +dP/dt 3884±104 mmHg/s; -dPdt = -2798±120 mmHg/s and SVE = 110±0,7 mmHg) or Los (LVEDP = 16±2,9 mmHg; +dP/dt: 4146±131 mmHg/s; -dPdt = -2823±136 mmHg/s; SBP = 111±3,5 mmHg). The right ventricle hemodynamic revealed an increase in systolic pressure in the IM-Pla group (40±0,6 mmHg) with a small decrease in the IM group under DIZE (37±2 mmHg). The IM-DIZE (0,33±0,03 mmHg/mL e 0,64±0,01 mmHg/mL) and IM-Los (0,36±0,03 mmHg/mL e 0,65±0,04 mmHg/mL) groups showed less left ventricular dilatation and stiffness as compared with the infarcted group under Pla (0,39±0,03 mmHg/mL e 0,78±0,02 mmHg/mL). The volumetric fraction of collagen in the surviving left ventricular myocardium increased, was partially prevented by DIZE or Los treatment. The postinfarction hypertrophy of cardiomyocytes, however, remained unaffected by DIZE treatment. As expected, treatment with losartan attenuated the hypertrophic growth in the left ventricle. In conclusion, our study showed that DIZE was effective to partially prevent the hemodynamic changes induced by infarction in rats similarly to the observation in infracted rats treated with Los. The two drugs also prevented the increase in the collagen deposition in the surviving left ventricular myocardium. In relation to the hypertrophic of cardiomyocytes, however, only Los showed a preventive effect.
publishDate 2016
dc.date.issued.fl_str_mv 2016-09-29
dc.date.accessioned.fl_str_mv 2018-08-01T22:58:25Z
dc.date.available.fl_str_mv 2018-08-01
2018-08-01T22:58:25Z
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Mestrado em Ciências Fisiológicas
dc.publisher.program.fl_str_mv Programa de Pós-Graduação em Ciências Fisiológicas
dc.publisher.initials.fl_str_mv UFES
dc.publisher.country.fl_str_mv BR
dc.publisher.department.fl_str_mv Centro de Ciências da Saúde
publisher.none.fl_str_mv Universidade Federal do Espírito Santo
Mestrado em Ciências Fisiológicas
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