A novel quantification of the relationship between blood sugar and stress / Y.J. Chen

Chen, Yi-Ju

January 2008

The rapid growth of biotechnology has promoted industries to harness the market in the field of human energy systems. A growing literature of research has linked human energy systems to weight loss, major diseases or illnesses. In our modern society, the general public is exposed to everyday stress, which often results in the development of chronic stress. Therefore, stress becomes an important area of medicine. It has been postulated that suppressing these physiological responses may help in disease prevention. Consequently, there is an urge for defining a model integrating stress with the human energy model. Over the past decades, a large amount of research has been put forward in defining the physiological responses or changes when an individual experiences psychological or environmental changes such as interpersonal dysfunction, traumatic experiences and diseases. Interestingly, it reveals that blood glucose fluctuation tends to be the end product of most psychological or physiological stressors. The blood glucose system is one of the major subsystems of the complete metabolic fuel system in humans. In this study, an empirical model and procedure for the derivation of the model due to various psychological influences on the human energy system are presented. This study can be divided into two main sections. An overview of a previously developed unit (ets: equivalent teaspoon sugar) for blood glucose quantification is given in the first section. Stress quantification methods are derived in the second section and a link between these methods and ets is drawn. A verification study of the derived model is also presented in the second section. Stress can be divided into physiological stress and psychological stress. Between the two types of stress, a generalised model based on studies of physiological stress has been drawn and accepted by the public. However, the generalised model does not account for psychological stress. Evidence shows that depending on the specific nature of a stressful circumstance, it can cause different activations of central circuits leading to the release of different neurotransmitters. However, these neurotransmitters have a common effect of increasing blood glucose concentrations. A substantial amount of literature shows that, when stress involves mental effort, epinephrine (EPI) is the main endocrine response. However, stress that does not require mental effort mainly induces cortisol release. The response models for different types of stress were derived using these relations. Furthermore, it is known that prolonged stress may lead to the development of disease. Several studies have used this observation and associated chronic stress with the relative risk factor of cardiovascular disease (CVD). Previously, different quartiles of risk factors for CVD have been related to blood glucose energy and ets expenditure. This link was further utilised to quantify chronic stress in this study. Increases in either of the two endocrine concentrations have been shown to raise the blood glucose level. In order to demonstrate the benefits of applying the ets concept, the cortisol and epinephrine responses were further quantified using the new glucose quantification method, the equivalent teaspoon sugar (ets) concept. The models derived in this study were verified against measured data. The models reveal a strong agreement with the measured data and therefore support the feasibility of these quantification methods. In conclusion, a link does exist between blood glucose energy and stress, and the highly accurate models derived for this association may serve as an adjunct tool for glycaemic control and stress management. / Thesis (Ph.D. (Electronical Engineering))--North-West University, Potchefstroom Campus, 2008.

Acute stress

Blood glucose

Cardiovascular disease

Chronic stress

Cortisol

Diabetes

Energy expenditure

Epinephrine

Equivalent teaspoon sugar

Hypothalamo-pituitary-adrenocortical

Insulin

Psychological stress

Relative risk factor

Sympathetic nervous system

A novel quantification of the relationship between blood sugar and stress / Y.J. Chen

Chen, Yi-Ju

January 2008

The rapid growth of biotechnology has promoted industries to harness the market in the field of human energy systems. A growing literature of research has linked human energy systems to weight loss, major diseases or illnesses. In our modern society, the general public is exposed to everyday stress, which often results in the development of chronic stress. Therefore, stress becomes an important area of medicine. It has been postulated that suppressing these physiological responses may help in disease prevention. Consequently, there is an urge for defining a model integrating stress with the human energy model. Over the past decades, a large amount of research has been put forward in defining the physiological responses or changes when an individual experiences psychological or environmental changes such as interpersonal dysfunction, traumatic experiences and diseases. Interestingly, it reveals that blood glucose fluctuation tends to be the end product of most psychological or physiological stressors. The blood glucose system is one of the major subsystems of the complete metabolic fuel system in humans. In this study, an empirical model and procedure for the derivation of the model due to various psychological influences on the human energy system are presented. This study can be divided into two main sections. An overview of a previously developed unit (ets: equivalent teaspoon sugar) for blood glucose quantification is given in the first section. Stress quantification methods are derived in the second section and a link between these methods and ets is drawn. A verification study of the derived model is also presented in the second section. Stress can be divided into physiological stress and psychological stress. Between the two types of stress, a generalised model based on studies of physiological stress has been drawn and accepted by the public. However, the generalised model does not account for psychological stress. Evidence shows that depending on the specific nature of a stressful circumstance, it can cause different activations of central circuits leading to the release of different neurotransmitters. However, these neurotransmitters have a common effect of increasing blood glucose concentrations. A substantial amount of literature shows that, when stress involves mental effort, epinephrine (EPI) is the main endocrine response. However, stress that does not require mental effort mainly induces cortisol release. The response models for different types of stress were derived using these relations. Furthermore, it is known that prolonged stress may lead to the development of disease. Several studies have used this observation and associated chronic stress with the relative risk factor of cardiovascular disease (CVD). Previously, different quartiles of risk factors for CVD have been related to blood glucose energy and ets expenditure. This link was further utilised to quantify chronic stress in this study. Increases in either of the two endocrine concentrations have been shown to raise the blood glucose level. In order to demonstrate the benefits of applying the ets concept, the cortisol and epinephrine responses were further quantified using the new glucose quantification method, the equivalent teaspoon sugar (ets) concept. The models derived in this study were verified against measured data. The models reveal a strong agreement with the measured data and therefore support the feasibility of these quantification methods. In conclusion, a link does exist between blood glucose energy and stress, and the highly accurate models derived for this association may serve as an adjunct tool for glycaemic control and stress management. / Thesis (Ph.D. (Electronical Engineering))--North-West University, Potchefstroom Campus, 2008.

Acute stress

Blood glucose

Cardiovascular disease

Chronic stress

Cortisol

Diabetes

Energy expenditure

Epinephrine

Equivalent teaspoon sugar

Hypothalamo-pituitary-adrenocortical

Insulin

Psychological stress

Relative risk factor

Sympathetic nervous system

Sympathikusaktivität bei handchirurgischen Operationen mit axillärer Plexus- oder Allgemeinanästhesie / Activity of the sympathetic nervous system of patients undergoing hand surgery under axillary plexus blockade (axPlex) or general anesthesia (ITN)

Klaholz, Andreas Manfred

12 February 2014

Ziel dieser Studie war die Messung der Symphatikusaktivität als Indikator einer Stressreaktion bei handchirurgischen Eingriffen. Zwei Gruppen á 23 Patienten (Alter [Jahre] ITN 21-76(51) axPlex 27-66(52) p=0,73; BMI ITN 18,2-40,3(26,4) axPlex 20,9-34,9(25,5) p=0,97), die sich in ultraschallgesteuerter axillärer Plexusblockade (axPlex) oder Allgemeinanästhesie (ITN) einer Operation unterziehen mussten, wurden nach Genehmigung durch die Ethikkommission untersucht. Ausschlusskriterien waren ein Alter < 18 Jahre oder > 80 Jahre, eine ASA-Klassifikation > III, sowie eine Kontraindikation gegen die verwendeten Medikamente oder Narkosenformen. Die Symphatikusaktivität wurde anhand des Hautwiderstands (ESG® 1001, Ingenieurbüro Dr.Janitzki, Altenbeken, Germany) gemessen. Die Herzfrequenz (HF), der non invasive Blutdruck und die Hauttemperatur wurden erfasst. Die Messung umfasste sieben Zeitpunkte (T-Ausgangswert, T-Narkosebeginn, T-Blutsperre, T-Schnitt, T-OP-Ende, T-Aufwachraum, T-Normalstation). Die Narkosetiefe der ITN wurde mit BIS® (40-60) überwacht. Die Analyse zeigte signifikante Unterschiede zwischen beiden Gruppen. In Bezug auf die Sympathikusaktivität konnte kein Unterschied zwischen beiden Gruppen gefunden werden.

610

Sympathikusaktivität

Hautwiderstand

axilläre Plexusanästhesie

sympathetic nervous system

skin resistance

axillary plexus blockade

Cell therapy for spinal cord injury, studies of motor and sensory systems /

Hofstetter, Christoph,

January 2005

Diss. (sammanfattning) Stockholm : Karolinska institutet, 2005. / Härtill 6 uppsatser.

Neurotrophin expression in sympathetic neurons influences of exogenous NGF and afferent input /

Jones, Elizabeth Ellen.

January 2004

Thesis (M.S.)--Miami University, Dept. of Zoology, 2004. / Title from first page of PDF document. Includes bibliographical references (p. 36-47).

Efeitos do beta-bloqueador bucindolol na modulação do remodelamento do ventrículo direito em modelo de hipertensão pulmonar induzida por monocrotalina

Seolin, Bruna Gazzi de Lima

January 2015

A hipertensão arterial pulmonar (HAP) é caracterizada pelo aumento da resistência vascular pulmonar (RVP). Em decorrência, há elevação da pós-carga imposta ao ventrículo direito (VD) e hipertrofia. Assim, com aumento de consumo de O2 pelo miocárdio, é provável que o estresse oxidativo esteja participando do desenvolvimento e progressão desta doença. Sabe-se que o bloqueio beta-adrenérgico diminui a mortalidade de pacientes com insuficiência cardíaca à esquerda, porém pouquíssimas pesquisas referem sua utilização na insuficiência cardíaca à direita. O bucindolol é um beta-bloqueador que atua nos receptores β1, β2, α1 e com propriedade simpatolítica. O objetivo deste estudo foi testar a hipótese de que o tratamento com bucindolol poderia reduzir a hipertrofia do VD e melhorar a função sistólica e diastólica do miocárdio. Foram utilizados ratos Wistar machos pesando 130±10 gramas divididos em quatro grupos (n=7-10/grupo): monocrotalina sem bucindolol (MCT SEM BCD), monocrotalina bucindolol (MCT+BCD), controle sem bucindolol (CTR SEM BCD) e controle bucindolol (CTR+BCD). A HAP foi induzida por meio de uma dose única de monocrotalina (60 mg/Kg – i.p.). Após duas semanas, os animas foram tratados por sete dias com bucindolol (2 mg/Kg/dia – i.p.) ou veículo. No 22º dia após a administração da monocrotalina, os animais foram anestesiados (i.p.) com quetamina (90 mg/Kg) e xilazina (10 mg/Kg), submetidos à ecocardiografia, cateterismo da artéria femoral, cateterismo do VD e decapitados, com posterior coleta dos tecidos. Os resultados foram avaliados utilizando ANOVA de duas vias (Sigma Plot 12.0) seguida pelo 8 teste de Student-Newman-Keuls, com nível de significância P<0,05. Os resultados serão apresentados na versão completa desta dissertação. / Pulmonary arterial hypertension is a rapidly progressive disease with poor prognosis, characterized by increase in pulmonary vascular resistance. As a result, there is an elevation of afterload imposed to the right ventricle and hypertrophy. Thus, since there is a rise in myocardial oxygen consumption, it is probable that oxidative stress is contributing to the development and progression of this disease. It is known that beta-adrenergic blockade reduces mortality in patients with left ventricular heart failure, but limited studies relate their use in right ventricular heart failure. The bucindolol is a beta-blocker that acts on receptors β1, β2, α1 and presents sympatholytic property. The aim of this study was to test the hypothesis that treatment with bucindolol could reduce right ventricular hypertrophy and improve systolic and diastolic function of the myocardium. Male Wistar rats weighing 130±10 grams were divided into four groups (n=7-10/group): monocrotaline without bucindolol (MCT WITHOUT BCD), monocrotaline bucindolol (MCT+BCD), control without bucindolol (CTR WITHOUT BCD) and control bucindolol (CTR+BCD). Pulmonary arterial hypertension was induced by a single dose of monocrotaline (60 mg/Kg – i.p.). After two weeks, the animals were treated for seven days with bucindolol (2 mg/Kg/day – i.p.) or vehicle. Twenty-two days after administration of monocrotaline, the animals were anesthetized intraperitoneally with ketamine (90 mg/Kg) and xylazine (10 mg/Kg), underwent echocardiography, catheterization of the femoral artery and of the right ventricle, decapitation and subsequent collection of tissues (heart, lungs, liver and tibia). The results were analyzed using two-way ANOVA (Sigma Plot 12.0) followed by 10 Student-Newman-Keuls test, with P<0.05 of significance level. Results will be presented in the full version.

Antagonistas adrenérgicos beta

Hipertensão pulmonar

Remodelação ventricular

Ventrículos do coração

Insuficiência cardíaca

Monocrotalina

Pulmonary hypertension

Sympathetic nervous system

Right heart failure

Beta-blocker

Bucindolol

Avaliação temporal da função vascular em aorta de camundongos com deleção dos receptores <font face=\"symbol\">a2A e <font face=\"symbol\">a2BC adrenérgicos. / Time-dependent characterization of vascular reactivity in aorta of <font face=\"symbol\">a2A and <font face=\"symbol\">a2C-adrenoceptors knockout mice.

Gisele Kruger Couto

10 September 2007

Este estudo avaliou a função vascular em anéis de aorta e no leito vascular mesentérico (LVM) de camundongos com deleção dos receptores <font face=\"symbol\">a2A e <font face=\"symbol\">a2Cadrenérgicos (KO) com 3, 5 e 7 meses, os quais apresentam uma hiperatividade simpática acompanhada de cardiomiopatia. Os KO apresentaram um aumento da freqüência cardíaca em todos os grupos avaliados, e hipertrofia ventricular esquerda aos 5 e 7 meses. Na aorta, o relaxamento dependente (acetilcolina) e independente (nitroprussiato de sódio) do endotélio e da via font face=\"symbol\">a-adrenérgica (isoproterenol), assim como a contração (fenilefrina e serotonina) e a mobilização de Ca2+ não foram alterados nos KO aos 3, 5 e 7 meses. Nos KO aos 3 meses, o relaxamento mediado pelos receptores ?2-adrenérgicos (clonidina) foi reduzido. Tanto a contração (noradrenalina) como o relaxamento (acetilcolina) no LVM dos KO aos 7 meses não foi alterado. Assim, sugere-se que os vasos arteriais parecem ser menos sensíveis do que o coração aos efeitos crônicos da hiperatividade simpática nos camundongos com deleção dos receptores <font face=\"symbol\">a2A e <font face=\"symbol\">a2C adrenérgicos. / This study assed the vascular function in aortic rings and in mesenteric vascular bed (MVB) from mice with disruption of <font face=\"symbol\">a2A and <font face=\"symbol\">a2Cadrenoceptors (KO) with 3, 5 and 7 months of age, that present sympathetic hyperactivity associated with cardiomyopathy. Heart rate was increased in all KO groups, and left ventricular hypertrophy was observed only in 5 and 7 month-old KO. There are no changes in the relaxation induced by acetylcholine (ACh), sodium nitroprusside and isoproterenol in aortic rings from all groups. In addition, the contraction induced by phenylephrine and serotonin, and Ca2+ handling did not change. However, in aorta from 3 month-old KO the relaxation induced by clonidine (<font face=\"symbol\">a2-adrenergic agonist) was reduced. In MVB from 7 month-old KO, neither the contraction (noradrenaline) nor relaxation (ACh) was modified. The results suggest that arterial vessel has been more resistant than heart to chronic effects induced by sympathetic hyperactivity observed in mice with disruption o<font face=\"symbol\">a2A and <font face=\"symbol\">a2C-adrenoceptors.

Aorta torácica

Camundongos

Endotélio vascular

Fisiologia cardiovascular

Receptores adrenérgicos

Sistema nervoso simpático

Adrenergic receptors

Cardiovascular physiology

Mice

Sympathetic Nervous system

Thoracic aortic

Vascular endothelium

Influência do sistema nervoso simpático na periodontite induzida e em glândula salivar de ratos

Martins, Luana Galvão [UNESP]

29 June 2011

Made available in DSpace on 2014-06-11T19:27:55Z (GMT). No. of bitstreams: 0 Previous issue date: 2011-06-29Bitstream added on 2014-06-13T19:15:37Z : No. of bitstreams: 1 martins_lg_me_sjc.pdf: 695176 bytes, checksum: fb089e33ad4b62aa9c5866bfb90390b7 (MD5) / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / Universidade Estadual Paulista (UNESP) / A ação de beta-bloqueadores na melhoria da qualidade óssea e sua ação anti-inflamatória embasam a hipótese de que a modulação simpática pode influenciar a evolução da doença periodontal (DP). Estudos demonstram relação entre disfunção salivar e DP; no entanto, os efeitos da DP nas glândulas salivares, cuja secreção é controlada pelo sistema nervoso autônomo, são pouco estudados. Objetivou-se analisar os efeitos do bloqueio e da ativação de receptores beta-adrenérgicos na reabsorção alveolar na DP em ratos, assim como os efeitos da DP, associada ou não a tratamento adrenérgico, nas glândulas salivares. Foram utilizados 40 ratos divididos em quatro grupos: (1) Grupo Propranolol 0,1mg/Kg com indução de DP; (2) Grupo Isoproterenol 0,75mg/Kg e DP; (3) Grupo Controle sem DP, com administração solução fisiológica ; (4) Grupo Controle com DP, com administração solução fisiológica. Depois de 14 dias de tratamento, ocorreu a eutanásia. Removeram-se as hemimandíbulas e as glândulas submandibulares e sublinguais para análise. O suporte e a perda óssea alveolar foram determinados radiográfica e macroscopicamente. As glândulas foram pesadas, medidas e submetidas à preparação de rotina para coloração com hematoxilina e eosina e Alcian Blue. Avaliou-se histomorfometricamente a área de ácinos, ductos e a vacuolização celular. Após estatística (p<0,05), verificou-se menor suporte e maior perda alveolar na presença de ligadura e maior perda alveolar em animais com tratados com isoproterenol. O isoproterenol aumentou significantemente peso e dimensões glandulares, reduziu área ductal e vacuolização, e aumentou área acinar na submandibular. Propranolol apenas reduziu vacuolização em relação ao controle com DP, e as demais comparações não foram estatisticamente significantes... / The action of beta-blockers in the improvement of bone quality and their anti-inflammatory actions base the hypothesis that sympathetic nervous system modulation can influence periodontal disease (PD). Studies demonstrate a relationship between salivary dysfunction and PD; however, there are few studies about the effects of PD in salivary glands, whose secretion is controlled by the autonomic nervous system. The aim of this study was to analyze the effects of the blockade and of the activation of beta-adrenergic receptors in alveolar resorption in PD in rats, as well as the effects of PD, associated or not to adrenergic treatment, in salivary glands. Forty rats were divided into four groups: (1) group Propranolol 0.1mg/Kg with PD induction; (2) group Isoproterenol 0.75mg/Kg and PD; (3) group Control without PD, which received saline; (4) group Control with PD, which also received saline. After 14 days of treatment, euthanasia occurred. Hemimandibles and submandibular and sublingual glands were removed for analysis. Alveolar bone support and alveolar bone loss were evaluated by radiographic and macroscopic analysis. Gland weight and dimensions were measured, and then the samples were submitted to routine preparation for hematoxilin and eosin and Alcian blue stainings. Acinar and ductal area and cellular vacuolization were histomorphometrically evaluated. After statistical analysis (p <0.05), less alveolar bone support and larger alveolar loss were verified in animals with ligatures for PD induction and larger alveolar loss were also verified in rats treated with isoproterenol. Isoproterenol also increased significantly glandular weight, size and acinar area, and reduced ductal area and cellular vacuolization in submandibular glands. Group Propranolol presented less vacuolization than group Control with DP... (Complete abstract click electronic access below)

Sistema nervoso simpatico

Receptores nervosos

Glandula submandibular

Periodontite

Glandulas salivares

Receptores adrenérgicos

Propranolol

Isoproterenol

Sympathetic nervous system

Adrenergic receptors

Submandibular gland

Efeitos do beta-bloqueador bucindolol na modulação do remodelamento do ventrículo direito em modelo de hipertensão pulmonar induzida por monocrotalina

Seolin, Bruna Gazzi de Lima

January 2015

A hipertensão arterial pulmonar (HAP) é caracterizada pelo aumento da resistência vascular pulmonar (RVP). Em decorrência, há elevação da pós-carga imposta ao ventrículo direito (VD) e hipertrofia. Assim, com aumento de consumo de O2 pelo miocárdio, é provável que o estresse oxidativo esteja participando do desenvolvimento e progressão desta doença. Sabe-se que o bloqueio beta-adrenérgico diminui a mortalidade de pacientes com insuficiência cardíaca à esquerda, porém pouquíssimas pesquisas referem sua utilização na insuficiência cardíaca à direita. O bucindolol é um beta-bloqueador que atua nos receptores β1, β2, α1 e com propriedade simpatolítica. O objetivo deste estudo foi testar a hipótese de que o tratamento com bucindolol poderia reduzir a hipertrofia do VD e melhorar a função sistólica e diastólica do miocárdio. Foram utilizados ratos Wistar machos pesando 130±10 gramas divididos em quatro grupos (n=7-10/grupo): monocrotalina sem bucindolol (MCT SEM BCD), monocrotalina bucindolol (MCT+BCD), controle sem bucindolol (CTR SEM BCD) e controle bucindolol (CTR+BCD). A HAP foi induzida por meio de uma dose única de monocrotalina (60 mg/Kg – i.p.). Após duas semanas, os animas foram tratados por sete dias com bucindolol (2 mg/Kg/dia – i.p.) ou veículo. No 22º dia após a administração da monocrotalina, os animais foram anestesiados (i.p.) com quetamina (90 mg/Kg) e xilazina (10 mg/Kg), submetidos à ecocardiografia, cateterismo da artéria femoral, cateterismo do VD e decapitados, com posterior coleta dos tecidos. Os resultados foram avaliados utilizando ANOVA de duas vias (Sigma Plot 12.0) seguida pelo 8 teste de Student-Newman-Keuls, com nível de significância P<0,05. Os resultados serão apresentados na versão completa desta dissertação. / Pulmonary arterial hypertension is a rapidly progressive disease with poor prognosis, characterized by increase in pulmonary vascular resistance. As a result, there is an elevation of afterload imposed to the right ventricle and hypertrophy. Thus, since there is a rise in myocardial oxygen consumption, it is probable that oxidative stress is contributing to the development and progression of this disease. It is known that beta-adrenergic blockade reduces mortality in patients with left ventricular heart failure, but limited studies relate their use in right ventricular heart failure. The bucindolol is a beta-blocker that acts on receptors β1, β2, α1 and presents sympatholytic property. The aim of this study was to test the hypothesis that treatment with bucindolol could reduce right ventricular hypertrophy and improve systolic and diastolic function of the myocardium. Male Wistar rats weighing 130±10 grams were divided into four groups (n=7-10/group): monocrotaline without bucindolol (MCT WITHOUT BCD), monocrotaline bucindolol (MCT+BCD), control without bucindolol (CTR WITHOUT BCD) and control bucindolol (CTR+BCD). Pulmonary arterial hypertension was induced by a single dose of monocrotaline (60 mg/Kg – i.p.). After two weeks, the animals were treated for seven days with bucindolol (2 mg/Kg/day – i.p.) or vehicle. Twenty-two days after administration of monocrotaline, the animals were anesthetized intraperitoneally with ketamine (90 mg/Kg) and xylazine (10 mg/Kg), underwent echocardiography, catheterization of the femoral artery and of the right ventricle, decapitation and subsequent collection of tissues (heart, lungs, liver and tibia). The results were analyzed using two-way ANOVA (Sigma Plot 12.0) followed by 10 Student-Newman-Keuls test, with P<0.05 of significance level. Results will be presented in the full version.

Antagonistas adrenérgicos beta

Hipertensão pulmonar

Remodelação ventricular

Ventrículos do coração

Insuficiência cardíaca

Monocrotalina

Pulmonary hypertension

Sympathetic nervous system

Right heart failure

Beta-blocker

Bucindolol

Efeitos do beta-bloqueador bucindolol na modulação do remodelamento do ventrículo direito em modelo de hipertensão pulmonar induzida por monocrotalina

Seolin, Bruna Gazzi de Lima

January 2015

A hipertensão arterial pulmonar (HAP) é caracterizada pelo aumento da resistência vascular pulmonar (RVP). Em decorrência, há elevação da pós-carga imposta ao ventrículo direito (VD) e hipertrofia. Assim, com aumento de consumo de O2 pelo miocárdio, é provável que o estresse oxidativo esteja participando do desenvolvimento e progressão desta doença. Sabe-se que o bloqueio beta-adrenérgico diminui a mortalidade de pacientes com insuficiência cardíaca à esquerda, porém pouquíssimas pesquisas referem sua utilização na insuficiência cardíaca à direita. O bucindolol é um beta-bloqueador que atua nos receptores β1, β2, α1 e com propriedade simpatolítica. O objetivo deste estudo foi testar a hipótese de que o tratamento com bucindolol poderia reduzir a hipertrofia do VD e melhorar a função sistólica e diastólica do miocárdio. Foram utilizados ratos Wistar machos pesando 130±10 gramas divididos em quatro grupos (n=7-10/grupo): monocrotalina sem bucindolol (MCT SEM BCD), monocrotalina bucindolol (MCT+BCD), controle sem bucindolol (CTR SEM BCD) e controle bucindolol (CTR+BCD). A HAP foi induzida por meio de uma dose única de monocrotalina (60 mg/Kg – i.p.). Após duas semanas, os animas foram tratados por sete dias com bucindolol (2 mg/Kg/dia – i.p.) ou veículo. No 22º dia após a administração da monocrotalina, os animais foram anestesiados (i.p.) com quetamina (90 mg/Kg) e xilazina (10 mg/Kg), submetidos à ecocardiografia, cateterismo da artéria femoral, cateterismo do VD e decapitados, com posterior coleta dos tecidos. Os resultados foram avaliados utilizando ANOVA de duas vias (Sigma Plot 12.0) seguida pelo 8 teste de Student-Newman-Keuls, com nível de significância P<0,05. Os resultados serão apresentados na versão completa desta dissertação. / Pulmonary arterial hypertension is a rapidly progressive disease with poor prognosis, characterized by increase in pulmonary vascular resistance. As a result, there is an elevation of afterload imposed to the right ventricle and hypertrophy. Thus, since there is a rise in myocardial oxygen consumption, it is probable that oxidative stress is contributing to the development and progression of this disease. It is known that beta-adrenergic blockade reduces mortality in patients with left ventricular heart failure, but limited studies relate their use in right ventricular heart failure. The bucindolol is a beta-blocker that acts on receptors β1, β2, α1 and presents sympatholytic property. The aim of this study was to test the hypothesis that treatment with bucindolol could reduce right ventricular hypertrophy and improve systolic and diastolic function of the myocardium. Male Wistar rats weighing 130±10 grams were divided into four groups (n=7-10/group): monocrotaline without bucindolol (MCT WITHOUT BCD), monocrotaline bucindolol (MCT+BCD), control without bucindolol (CTR WITHOUT BCD) and control bucindolol (CTR+BCD). Pulmonary arterial hypertension was induced by a single dose of monocrotaline (60 mg/Kg – i.p.). After two weeks, the animals were treated for seven days with bucindolol (2 mg/Kg/day – i.p.) or vehicle. Twenty-two days after administration of monocrotaline, the animals were anesthetized intraperitoneally with ketamine (90 mg/Kg) and xylazine (10 mg/Kg), underwent echocardiography, catheterization of the femoral artery and of the right ventricle, decapitation and subsequent collection of tissues (heart, lungs, liver and tibia). The results were analyzed using two-way ANOVA (Sigma Plot 12.0) followed by 10 Student-Newman-Keuls test, with P<0.05 of significance level. Results will be presented in the full version.

Antagonistas adrenérgicos beta

Hipertensão pulmonar

Remodelação ventricular

Ventrículos do coração

Insuficiência cardíaca

Monocrotalina

Pulmonary hypertension

Sympathetic nervous system

Right heart failure

Beta-blocker

Bucindolol