Estudo dos mecanismos neuronais hipotalâmicos e bulbares envolvidos no modelo de hipertensão induzida por sobrecarga de sódio. / Hypothalamic and medullary pathways involved in sodium-induced hypertension.

Ribeiro, Natalia

20 July 2018

O aumento da osmolaridade plasmática é conhecido como hiperosmolaridade e é resultado do aumento do aporte de sódio ou, da diminuição do volume plasmático de água. Trata-se de um desafio orgânico capaz de iniciar uma série de respostas neuro-hormonais que incluem a liberação de vasopressina e aumento da atividade simpática, com consequente elevação da pressão arterial. Descrever o papel do sistema nervoso autonômico no desenvolvimento da hipertensão arterial secundária a ingestão de sódio é essencial para elucidar os mecanismos envolvidos na gênese desta patologia. Neste sentido, o RVLM é um importante alvo de estudos, dado seu envolvidos na regulação da atividade simpática, via projeções para a CIML. O RVLM possui um grupo neuronal denominado C1 caracterizado pela presença da enzima PNMT; a ativação destes neurônios já foi descrita em resposta a diversos desafios orgânicos tais como hipóxia, dor, hemorragia, inflamação, hipotensão e hipoglicemia. Sendo a hiperosmolaridade um desequilíbrio da homeostase propusemos investigar a possível participação dos neurônios adrenérgicos do grupamento C1 sobre a hipertensão secundária ao desafio hiperosmótico desencadeado pela ingestão crônica de solução de 2% cloreto de sódio (salina hipertônica de NaCl 2%) por 7 dias. Nossos resultados nos permitem concluir que: 1) a injeção de anti-D&betaH-saporina na região do RVLM causou a depleção de neurônios TH+ nas regiões C1 e A5; 2) A depleção dos neurônios TH+ não alterou o comportamento de ingestão de sódio e, tampouco os valores de hematócrito e osmolaridade plasmática resultados da exposição ao hiperosmótico durante 7 dias, comparado aos animais controle; 3) A lesão prévia dos neurônios do C1 e A5 inibe o desenvolvimento da hipertensão secundária ao estímulo hiperosmótico por ingestão de NaCl 2%. Além disso, propusemos também estudar como estariam as respostas cardiovasculares e de controle hidroeletrolítico em indivíduos normotensos e previamente hipertensos frente a diferentes intensidades de estímulo hiperosmótico desencadeado pela ingesta de salina hipertônica de NaCl 2%. Os resultados demonstraram que 1) a ingestão de sódio desencadeia uma elevação da pressão arterial de maior magnitude nos SHR, quando comparado aos animais Wistar; 2) que não parece estar envolvida com diferenças no balanço hidroeletrolítico, uma vez que observou-se repostas similares entre as duas linhagens; 3) houve ainda, um aumento da expressão do RNAm para neuropeptídeo vasopressina (VP) no núcleo paraventricular do hipotálamo (PVN) tanto em Wistar quanto em SHR decorrente da ingestão de NaCl 2% durante 7 dias. Até o presente momento nossos resultados permitem duas considerações acerca dos mecanismos envolvidos nas repostas geradas frente desafios da osmolaridade: 1) os neurônios TH+ e, potencialmente do grupamento C1, estão envolvidos no desenvolvimento da hipertensão arterial em situações de desafio crônico da osmolaridade; 2) em animais hipertensos (SHR) o estímulo hiperosmótico gera uma elevação da pressão arterial de maior magnitude em comparação aos animais normotensos, fato que sugerimos envolver mecanismos de controle neural da pressão arterial, uma vez que não se observou alterações significativas nos parâmetros hidroeletrolítico e função renal entre as duas linhagens. / Plasma osmolarity increases is known as hyperosmolarity and it is a consequence of high sodium intake or decrease of water plasma content. It is an organic imbalance that elicits neurohormonal responses including release of vasopressin and increased in sympathetic activity, with consequent elevation of blood pressure. To describe the role of the autonomic nervous system in the development of sodium induced hypertension is critical to elucidate the mechanisms involved in the genesis of this pathology. In this sense, the RVLM is an important target, given its involved in the regulation of sympathetic activity, via CIML projections. The RVLM has a neuronal group known as C1 that present the PNMT enzyme; the activation of these neurons has already been described in response to several organic challenges such as hypoxia, pain, hemorrhage, inflammation, hypotension and hypoglycemia. Since hyperosmolarity is an homeostasis imbalance, we propose to investigate the role of adrenergic C1 neurons on sodium induced hypertension, triggered by the chronic ingestion of NaCl2% solution during 7 days. Our results allow us to conclude that: 1) the anti-D&betaH-saporin injection in the RVLM led to a depletion of TH+ neurons in the C1 and A5 regions; 2) Depletion of TH + neurons did not alter the sodium intake behavior, hematocrit and plasma osmolality values result from 7 days NaCl 2% exposure, compared to control animals; 3) Depletion of TH+ in C1 and A5 regions inhibits the development of sodium induced hypertension . In addition, we also proposed to investigate the cardiovascular and hydroelectrolytic responses elicits in normotensive and hypertensive rats, in response to different intensities of hyperosmotic stimulation triggered by the ingestion of hypertonic saline of NaCl 2%. The results demonstrated that: 1) the increase in blood pressure triggers by NaCl 2% intake is higher in SHR when compared to Wistar animals; 2) that does not appear to be involved with differences in hydroelectrolyte balance, since similar responses were observed between the two strains; 3) there was also an increase in mRNA expression for neuropeptide vasopressin (VP) in the paraventricular nucleus of the hypothalamus (PVN) in both strains, Wistar and SHR, in consequence of 7 days NaCl 2% intake. Our results allow two considerations about the mechanisms involved in the responses elicits by osmolarity challenges: 1) TH+ neurons and, potentially C1 neurons, are involved in the development sodium induced hypertension and; 2) in SHRs the hyperosmotic stimulus generates a higher blood pressure increase in comparison to normotensive animals, which seems to be associated with sympathoexcitatory components, since no significant alterations were observed in the hydroelectrolytic parameters and renal function between the two strains.

The Cardiovascular Effects of alpha-Melanocyte-Stimulating Hormone in the Nucleus Tractus Solitarii of Spontaneously Hypertensive Rats

Weng, Wen-Tsan

09 August 2004

alpha-melanocyte stimulating hormone (alpha-MSH) is an important regulator of food intake, metabolic rate, and inflammation. Recently, alpha-MSH was shown to influence sympathetic activity and blood pressure regulation. In the present study, we investigated the cardiovascular effects of alpha-MSH in the nucleus tractus solitarii (NTS) of spontaneously hypertensive rats (SHR). Because nitric oxide (NO) is well-known to involve in central cardiovascular regulation, we elucidated the role of NO in the cardiovascular responses induced by alpha-MSH. In urethane-anesthetized SHR, unilateral microinjection of alpha-MSH (0.3-300 pmol) into the NTS produced dose-responsive depressor and bradycardic effects. The cardiovascular effects of alpha-MSH were abrogated by the antagonist of melanocortin receptor (MC3/4-R), SHU9119. Pretreatment with precursor of nitric oxide, L-arginine, enhanced the duration of alpha-MSH-mediated hypotensive effects, whereas prior application of L-NAME, a universal inhibitor of nitric oxide synthase (NOS), significantly attenuated the effects of alpha-MSH. Prior injection with inhibitor of inducible NOS, aminoguanidine, but not inhibitor of neuronal NOS, 7-nitroindazole, attenuated the hypotensive effect of alpha-MSH. In summary, these results indicated alpha-MSH induced depressor and bradycardic effects in the NTS of SHR. Besides, the hypotensive mechanism of alpha-MSH was mediated via MC4-R and involved with iNOS activation in the NTS of SHR.

spontaneously hypertensive rats (SHR)

nucleus tractus solitarii (NTS)

depressor and bradycardic effects

nitric oxide (NO)

melanocortin receptor

cardiovascular effect

alpha-melanocyte stimulating hormone

Influência do exercício físico no remodelamento cardíaco, estresse oxidativo e vias de sinalização das MAPK e do NF-κB de ratos espontaneamente hipertensos / Influence of physical exercise on cardiac remodeling, oxidative stress, MAPK and NF-kB pathways signaling in spontaneously hypertensive rats

Pagan, Luana Urbano

02 March 2018

Submitted by Luana Urbano Pagan null (luanapagan@alunos.fmb.unesp.br) on 2018-03-13T18:51:41Z No. of bitstreams: 1 Tese Doutorado 1 fev 2018 - Luana Urbano Pagan.pdf: 2756763 bytes, checksum: 6b255d0ba5900dbacc830d74916982d2 (MD5) / Approved for entry into archive by ROSANGELA APARECIDA LOBO null (rosangelalobo@btu.unesp.br) on 2018-03-16T19:35:20Z (GMT) No. of bitstreams: 1 pagan_lu_dr_bot.pdf: 2756763 bytes, checksum: 6b255d0ba5900dbacc830d74916982d2 (MD5) / Made available in DSpace on 2018-03-16T19:35:20Z (GMT). No. of bitstreams: 1 pagan_lu_dr_bot.pdf: 2756763 bytes, checksum: 6b255d0ba5900dbacc830d74916982d2 (MD5) Previous issue date: 2018-03-02 / Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP) / Introdução: A sobrecarga de pressão causada pela hipertensão arterial sistêmica (HAS) pode gerar mudança na arquitetura do colágeno, favorecer a fibrose, bem como o desbalanço entre a produção de espécies reativas de oxigênio (ERO) e a capacidade antioxidante. Aumento das ERO pode gerar ativação de vias sinalizadoras como a do fator nuclear kappa B (NF-kB) e das proteínas quinases ativadas por mitógenos (MAPK). Alterações dessas vias contribuem para o processo de remodelamento cardíaco causado pela HAS. O exercício físico desempenha importante papel na atenuação dos fatores de risco cardiovascular como a HAS. Dessa forma, o objetivo desse estudo foi avaliar a influência do treinamento físico sobre o remodelamento cardíaco de ratos espontaneamente hipertensos (SHR) na fase que antecede o desenvolvimento de insuficiência cardíaca. Métodos: Foram constituídos quatro grupos experimentais de ratos: normotensos Wistar (W) sedentários (W-SED, n=27); W exercitados (W-EX, n=31); SHR sedentários (SHR-SED, n=27); e SHR exercitados (SHR-EX, n=32). A partir de 13 meses de idade, os animais dos grupos exercitados foram submetidos a protocolo de exercício em esteira, cinco dias por semana, durante quatro meses. A avaliação estrutural e funcional in vivo do coração foi realizada por ecocardiograma. A função miocárdica in vitro foi avaliada em preparações de músculo papilar isolado do ventrículo esquerdo (VE). Amostras de tecido do VE foram obtidas para análises bioquímicas, histológicas e moleculares. A avaliação do colágeno miocárdico total foi realizada pela histologia e por quantificação de hidroxiprolina. O tamanho dos miócitos foi medido em cortes histológicos do VE. A atividade das enzimas antioxidantes foi quantificada por espectrofotometria. A atividade da NADPH oxidase foi avaliada pela redução da lucigenina. A quantificação proteica dos colágenos I e III, lisil oxidase, vias MAPK e NF-kB, e inibidores teciduais 1 e 2 das metaloproteinases foi realizada por Western blot. A atividade das metaloproteinases foi realizada por zimografia. As comparações entre os grupos foram realizadas por análise de variância (ANOVA) complementada pelo teste de Bonferroni (distribuição normal), ou o teste de Kruskal-Wallis complementado pelo teste de Dunn (distribuição não normal). Resultados: A pressão arterial sistólica foi maior nos grupos SHR. Os grupos exercitados apresentaram maior capacidade física. Os sinais de insuficiência cardíaca foram maiores nos grupos hipertensos em relação aos controles, e o grupo SHR-EX apresentou menor prevalência de derrame pleural e taquipneia em comparação ao SHR-SED. O ecocardiograma mostrou reduções da espessura da parede do VE, espessura relativa do VE, diâmetro do átrio esquerdo e melhora do relaxamento no grupo SHR-EX vs. SHR-SED. O estudo da função miocárdica in vitro mostrou melhor performance no grupo SHR-EX (derivada positiva da tensão desenvolvida) vs. SHR-SED. O grupo SHR-EX mostrou maior atividade das enzimas antioxidantes em comparação SHR-SED. A produção de hidroperóxido de lipídeo, diâmetros dos miócitos, expressões proteicas da JNK fosforilada e da IkB total foram maiores nos grupos hipertensos. A quantificação de hidroxiprolina, malondialdeído, atividade da NADPH oxidase, expressões proteicas do colágeno III, lisil oxidase, TIMP-1, JNK total, p38 fosforilada, p65 fosforilada e total e IkB fosforilada não apresentaram diferença entre os grupos. A fração colágena intersticial, a atividade da MMP-2 e a expressão proteica da p38 total, ERK total e fosforilada foram maiores no SHR-SED em comparação com controle. O exercício causou redução da atividade da MMP-2 e da expressão da ERK fosforilada nos ratos hipertensos. Conclusão: O exercício físico em ratos espontaneamente hipertensos atenua o remodelamento cardíaco que está associado à melhora da tolerância ao esforço físico e redução da frequência de sinais de insuficiência cardíaca. Além disso, associa-se ao aumento da atividade das enzimas antioxidantes, diminuição da fosforilação da ERK e da atividade da MMP-2, e atenuação da expressão proteica da ERK total. / Introduction: The pressure overload caused by systemic arterial hypertension (SAH) may change the collagen architecture, induce fibrosis, as well as imbalance between the reactive oxygen species (ROS) production and antioxidant capacity. Increased ROS leads to activation of signaling pathways such as nuclear factor kappa B (NF-kB) and mitogen-activated protein kinases (MAPK). Alterations in these pathways contribute to cardiac remodeling process induced by SAH. Physical exercise plays an important role in mitigating cardiovascular risk factors such as hypertension. Therefore, the aim of this study was to evaluate the influence of physical training, started before clinical evidence of heart failure, on cardiac remodeling in spontaneously hypertensive rats (SHR). Methods: Four experimental groups were used: sedentary (W-SED n=27) and trained (W-EX, n=31) normotensive Wistar rats, and sedentary (SHR-SED, n=27) and exercised (SHR-EX, n=32) hypertensive rats. Rats of the exercise groups underwent a protocol of treadmill exercise five days a week, for four months; exercise started at 13 months of age. Echocardiogram was performed to evaluate in vivo cardiac structures and function. In vitro myocardial function was analyzed in left ventricular (LV) papillary muscle preparations. LV tissue samples were obtained for biochemical, histological, and molecular analysis. Total myocardial collagen was assessed by histology and hydroxyproline quantification. Cardiomyocyte size was measured in LV histological sections. Antioxidant enzymes activity was quantified by spectrophotometry. NADPH oxidase activity was analyzed by reduction of lucigenin. Protein expression of collagen I and III, lysyl oxidase, MAPK and NF-kB, and metalloproteinases tissue inhibitors 1 and 2 was quantified by Western blot. The activity of metalloproteinases was evaluated by zymography. Comparisons between groups were performed by two factors analysis of variance (ANOVA), complemented with the Bonferroni test (normal distribution), or Kruskal-Wallis complemented with Dunn test (non-normal distribution). Results: Systolic blood pressure was higher in the SHR groups. The exercised groups showed greater physical capacity. Prevalence of heart failure signs was higher in the hypertensive groups compared to controls, and the SHR-EX group showed lower prevalence of pleural effusion and tachypnea compared to SHR-SED. Echocardiogram showed lower LV wall thickness, LV relative wall thickness, left atrium diameter, and relaxation time in the SHR-EX group vs. SHR-SED. Myocardial functional study showed better performance in the SHR-EX group (positive derivative of the developed tension) vs. SHR-SED. The SHR-EX group showed higher antioxidant enzymes activity compared to SHR-SED. Lipid hydroperoxide production, myocyte diameters, and phosphorylated JNK and total IkB protein expression were higher in the hypertensive groups. Quantification of hydroxyproline, malondialdehyde, NADPH oxidase activity, and protein expression of collagen III, lysyl oxidase, TIMP-1, total JNK, phosphorylated p38, phosphorylated and total p65, and phosphorylated IkB did not differ between groups. The interstitial collagen fraction, MMP-2 activity, protein expression of total p38, and total and phosphorylated ERK were higher in the SHR-SED group compared to normotensive control. Physical exercise reduced the MMP-2 activity and the phosphorylated ERK expression in hypertensive rats. Conclusion: Physical exercise in spontaneously hypertensive rats attenuates cardiac remodeling associated with improved physical capacity and reduced prevalence of heart failure signs. In addition, it is associated with increased antioxidant enzymes activity, decreased ERK phosphorylation and MMP-2 activity, and attenuation of total ERK protein expression. / FAPESP: 2014/00747-1

Exercício físico

Hipertensão arterial

Remodelamento cardíaco

Ratos espontaneamente hipertensos

Estresse oxidativo

Matriz extracelular

MAPK

NF-kB

Physical exercise

Arterial hypertension

Cardiac remodeling

Spontaneously hypertensive rats

Avaliação da atividade cardiovascular do extrato seco de própolis vermelha em ratos espontaneamente hipertensos / Evaluation of the cardiovascular activity of dry extract of red propolis in spontaneously hypertensive rats

Herculano, Edla de Azevedo

23 March 2017

Arterial hypertension it is the leading risk factor for cardiovascular disease. Its prevalence appears to be about 30-45% of the general population. Despite current knowledge the long-term adherence to cardiovascular drugs is still low in hypertension treatment. The Brazilian red propolis has a large content of phenols compounds such as isoflavones, this have been reported to exert beneficial effects in cardiovascular disease, including hypertension. Therefore the objective of this study was to investigate cardiovascular effects from a red propolis gastroretentive system (ESPV, patents register numbers BR 10 2012 013590-6 A2 and WO 2014/186851) in spontaneously hypertensive rats (SHR). The HPLC-UV analysis showed in ESPV chemical composition the presence propolis chemical markers: daidzein, biochanin A, liquiritigenin, pinobanksin, isoliquiritigenin, formononetin and pinocembrina. The cytotoxicity from ESPV was evaluate on macrophage J774 by MTT assay and exhibited IC50 = 72.86 μg/mL. Intravenous injection of ESPV caused a hipotensive dose-dependent effect at 0.1, 0.5, 1, 5 and 10 mg/kg, unchanges heart rate in conscious SHR. The hypotensive effect was not affected by anesthesia. In intact rings of rat mesenteric artery pre-contracted with 10 μM phenylephrine, ESPV induced relaxations (Emax = 100 ± 0.4 %; pD2 = 1.08 ± 0.02 μg/mL) that were affected by endothelium removal, (Emax = 56.7 ± 2 %; pD2 = 1.37 ± 0.04 μg/mL). In an antihypertensive study, ESPV (75 and 150 mg/kg) was orally administered to Juvenile (11-week-old) and young adult (24-week-old) SHRs, and the systolic pressure were measured using the tail-cuff method before and 7, 14, 21 and 28 days after beginning of treatment. Was observed a significant antihypertensive effect from 14th day of treatment only in young adult SHR, with decreased by 56 mmHg compared with baseline systolic blood pressure. Furthermore, the treatment reduced left ventricular hypertrophy in young adult SHR as evident by myocardial morphometry. The vascular function of mesenteric arteries was also investigated at the end of the treatment with ESPV in young adult SHR, the endothelium-independent relaxations to sodium nitroprusside (10-3 to 3.10-4 M) was unchanged compared to control. For other hand, endothelium-dependent relaxations to acetylcholine (10-3 to 3.10-4 M) was markedly improve (Emax = 76.4 ± 3.8% e pD2 = -8.72 ± 3.8 M). We therefore investigated vascular reactivity to acetylcholine (10-3 to 3.10-4 M) also in the presence of the nonspecific NOS inhibitor L-NAME (3.10-3 M), in order to assess NO-dependent relaxation. In these, relaxation response was abolished (Emax = 18.9 ± 1.65% e pD2 = -5.12 ± 0.33 M). Similary, the acetylcholine relaxation in the presence of L-NAME plus a cyclooxygenase antagonist, indomethacin (10-3 M), was too antagonized (Emax = 15.90 ± 1.32 % e pD2 = -5.39 ± 0.24 M), indicating that the response to ESPV treatement involves the enhancement of the nitric oxide via NOS relaxations. These results disclosed that ESPV is effective to lower blood pressure only of young adult SHR, its antihypertensive effect is associated with lowering left ventricular hypertrophy and probably by decrease peripheral vascular resistance, improving endothelial function and increasing the NO-dependent relaxation via NOS. / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Estima-se que hipertensão arterial é o principal fator de risco para doença cardiovascular. Sua prevalência parece ser cerca de 30-45% da população mundial. Contudo, apesar do conhecimento atual, a adesão ao tratamento da hipertensão a longo prazo ainda é baixa. A própolis vermelha brasileira apresenta grande teor de compostos fenólicos em sua constituição química, dentre os quais destacam-se as isoflavonas, metabólitos com efeitos benéficos para doenças cardiovasculares, incluindo hipertensão. Desta forma, o objetivo deste estudo foi investigar os efeitos cardiovasculares de um sistema gastrorresistente de própolis vermelha (ESPV, patentes registradas BR 10 2012 013590-6 A2 e WO 2014/186851) em ratos espontaneamente hipertensos (SHR). A análise HPLC-UV demonstrou a presença dos marcadores químicos para propolis na composição química do ESPV: daidzeína, biochanina A, liquiritigenina, pinobanksina, isoliquiritigenina, formononetina e pinocembrina. A avaliação da citotoxicidade de ESPV, em macrófagos J774 através do ensaio de MTT, revelou IC50 = 72,86 μg/mL. A injeção intravenosa de ESPV causou um efeito hipotensor dependente de dose (0,1; 0,5; 1; 5 e 10 mg/kg), sem alterar a freqüência cardíaca em SHR consciente. O efeito hipotensor não foi afetado pela anestesia. Em anéis de artéria mesentérica pré-contraídos com fenilefrina 10 μM, ESPV induziu vasorrelaxamento (Emax = 100 ± 0,4%; pD2 = 1,08 ± 0,02 μg/mL) que foi afetado pela remoção do endotélio (Emax = 56,7 ± 2%; PD2 = 1,37 ± 0,04 μg/mL). Na avaliação do efeito anti-hipertensivo, o ESPV (75 e 150 mg / kg) foi administrado oralmente a SHRs jovens (11 semanas de idade) e adultos jovens (24 semanas de idade), a pressão sistólica foi então avaliada através do método de medida indireta de pressão arterial tail-cuff antes e 7, 14, 21 e 28 dias após o início do tratamento. Desta forma, observou-se um efeito anti-hipertensivo significativo a partir do 14º dia de tratamento apenas em SHR de adultos jovens, com diminuição de 56 mmHg em comparação com a pressão arterial sistólica basal. Além disso, o tratamento reduziu a hipertrofia ventricular esquerda em SHR de adultos jovens como evidenciado pela morfometria miocárdica. Além disso, a função vascular das artérias mesentéricas de SHR tratados com SHR também foi investigada, o relaxamento independente do endotélio foi avaliado através de uma curva concentração-resposta para nitroprussiato de sódio (10-3 – 3.10-4 M), e sob estas condições permaneceram inalteradas em comparação ao controle. Por outro lado, o relaxamento dependentes do endotélio à avaliado através da curva para acetilcolina (10-3 – 3.10-4 M) apresentou melhorara significativa (Emax = 76,4 ± 3,8% e pD2 = -8,72 ± 3,8 M). Por conseguinte, para avaliar o relaxamento dependente de NO, investigou-se a reatividade vascular à acetilcolina (10-3 – 3.10-4 M) na presença do inibidor inespecífico de NOS, L-NAME (3.10-3 M). Nestas condições, a resposta relaxante foi abolida (Emax = 18,9 ± 1,65% e pD2 = -5,12 ± 0,33 M). Resultados similares, foram obtidos ao avaliar o relaxamento da acetilcolina na presença de L-NAME mais um antagonista da ciclo-oxigenase, a indometacina (10-3 M) (Emax = 15,90 ± 1,32% e pD2 = -5,39 ± 0,24 M), indicando que a resposta ao tratamento com ESPV envolve o aumento do relaxamento dependente de óxido nítrico via NOS. Estes resultados revelaram que o ESPV é eficaz para promover redução da pressão arterial apenas de SHR adultos jovens, que o efeito anti-hipertensivo está associado com a redução da hipertrofia ventricular esquerda e provavelmente pela diminuição da resistência vascular periférica, melhorando a função endotelial e aumentando o relaxamento dependente de NO através da NOS.

Própolis vermelha brasileira

Hipertensão

Disfunção endotelial

Brazilian red propolis

Hypertension

Endothelial dysfunction

SHR (Ratos Espontaneamente Hipertensos)

SHR (Spontaneously Hypertensive Rats)

Úloha mitochondrií v adaptaci na chronickou hypoxii u spontánně hypertenzních a konplastických potkanů / The role of mitochondria in adaptation to chronic hypoxia in the spontaneously hypertensive and conplastic rats.

Weissová, Romana

January 2013

Adaptation to chronic hypoxia provides cardioprotective effects. Molecular mechanism of this phenomenon is not yet completely understood, but it is known that cardiac mitochondria play an essential role in induction of protective effects. The purpose of this diploma thesis is to study effects of continuous normobaric hypoxia (CNH; 10 % O2, 21 days) on spontaneously hypertensive rats (SHR) and conplastic strain that is derived from SHR. These animals have nuclear genome of SHR strain and mitochondrial genome of Brown Norway (BN) strain. Cardiac homogenate was used to measure enzymatic activity of malate dehydrogenase (MDH), citrate synthase (CS), NADH-cytochrome c oxidoreductase, succinate-cytochrome c oxidoreductase and cytochrome oxidase (COX). Using Western blot procedure the protein amount of antioxidant enzymes was measured - manganese superoxide dismutase and copper-zinc superoxide dismutase (MnSOD, Cu/ZnSOD), catalase and chosen subunits of oxidative phosphorylation complexes (Ndufa9, Sdha, Uqcrc2, COX-4, MTCO1, Atp5a1). Under normoxic conditions the conplastic strain has lower amount of complex IV subunit MTCO1 in comparison with SHR. This subunit is encoded by mitochondrial DNA and it is one of the seven protein-coding genes in conplastic strain that differ from SHR. Adaptation to hypoxia causes an...

Effect of Tulbaghia violacea on the blood pressure and heart rate in male spontaneously hypertensive wistar rats

Raji, Ismaila

January 2011

<p>Tulbaghia violacea Harv. (Alliaceae) is a small bulbous herb which belongs to the family, Alliaceae, most commonly associated with onions and garlic. In South Africa (SA), this&nbsp / herb has been traditionally used in the treatment of various ailments, including fever, colds, asthma, paralysis, hypertension (HTN) and stomach problems. The aim of this study&nbsp / was to evaluate the effect of methanol leaf extracts (MLE) of T. violacea on the blood pressure (BP) and heart rate (HR) in anaesthetized male spontaneously hypertensive rats / &nbsp / and to find out the mechanism(s) by which it acts. The MLE of T. violacea (5 - 150 mg/kg), angiotensin I (ang I, 3.1 - 100 &mu / g/kg), captopril (10 mg/kg), angiotensin II (ang II, 3.1 - 50&nbsp / g/kg), losartan (30 mg/kg), phenylephrine (0.01 &ndash / 0.16 mg/kg), prazosin (1 mg/kg), dobutamine (0.2 &ndash / 10.0 &mu / g/kg), propranolol (0.1 - 12.8 mg/kg), muscarine (0.16 -10 &mu / g/kg),&nbsp / and atropine (0.02 - 20.48 mg/kg) were administered intravenously into male spontaneously hypertensive rats (SHR) weighing between 300 g and 350 g and aged less than 5&nbsp / months. The MLE of T. violacea and/or the standard drugs were infused alone, simultaneously, or separately into each animal. The BP and HR were measured via a pressure&nbsp / transducer connecting the femoral artery and the Powerlab. The vehicle (0.2 mls of a mixture of dimethylsulfoxide and normal saline), T. violacea (60 mg/kg) and captopril (10&nbsp / mg/kg) were injected intraperitoneally into some SHR for 21 days to investigate the chronic effect of these agents on plasma levels of aldosterone. The mean change, the mean&nbsp / of the individual percentage changes and the percentage difference (in mean) observed with each intervention was calculated and statistically analyzed using the Student&rsquo / s t test&nbsp / for significant difference (p &lt / 0.05). The Microsoft Excel software was used for statistical analysis. T. violacea significantly (p &lt / 0.05) reduced the systolic, diastolic, and mean&nbsp / arterial BP / and HR dose-dependently. In a dose-dependent manner, ang I, ang II, phenylephrine significantly (p &lt / 0.05) increased the BP, while propranolol, muscarine and&nbsp / atropine reduced the BP. The increases in BP due to dobutamine were not dose-dependent. In a dose dependent manner, phenylephrine and propranolol reduced the HR, while dobutamine increased the HR. The effect of ang I, ang II, muscarine and atropine on HR were not dose-dependent / with both increases as well as decreases observed with ang&nbsp / I, and II and atropine, while decreases were seen with muscarine. Captopril produced&nbsp / significant (p &lt / 0.05) reduction in BP which were not associated with any change in HR. The co-infusion of ang I with the MLE produced significant (p &lt / 0.05) reduction in BP, which were not associated with significant changes in HR. The co-infusion of ang II with the&nbsp / MLE did not produce any significant changes in BP or HR when compared to the infusion of the standard drug alone. The co-infusion of phenylephrine with the MLE did not&nbsp / produce any significant change in BP or HR when compared to the values obtained with the infusion of the standard drug alone, in both the absence and presence of prazosin.&nbsp / The co-infusion of dobutamine with T. violacea produced siginificant (p &lt / 0.05) increases in DBP which were associated with significant (p &lt / 0.05) reductions in HR, when&nbsp / compared to the values obtained with the infusion of the standard drug alone. Theco-infusion of atropine with the MLE did not produce any significant change in BP or HR when&nbsp / compared to the values obtained with the infusion of atropine alone. However, the infusion of T. violacea, 20 minutes after pre-treating animals with atropine (5.12 mg/kg) lead to&nbsp / dose dependent significant (p &lt / 0.05) increases in BP, which were associated with dose-dependent increases in HR. The chronic treatment of animals with T. violacea or&nbsp / captropril produced (a) signicant (p &lt / 0.05) reductions in the plasma levels of aldosterone when compared to the values obtained in the vehicle-treated group, (b) produced&nbsp / signifiant (p &lt / 0.05) reduction in BP in the captopril treated group when compared to the vehicle-treated, (c) did not produce any signficant change in BP in the T. violacea-treated&nbsp / group when compared to the vehicle-treated group and (d) did not produce any signifiant change in HR or body weight in any of the groups. The result obtained in this study&nbsp / suggests that T. violacea reduced BP and HR in the SHR. Secondly, the BP and HR reducing effect of the MLE may involve a) the inhibition of the ACE, b) the inhibition of the &beta / 1&nbsp / adrenoceptors, c) the stimulation of the muscarinic receptors and d) the reduction of the levels of aldosternone in plasma. The results also&nbsp / suggest that the MLE may not act&nbsp / through the angiotensin II receptors or the &alpha / 1 adrenergic receptors.&nbsp / </p>

Effect of Tulbaghia violacea on the blood pressure and heart rate in male spontaneously hypertensive wistar rats

Raji, Ismaila

January 2011

<p>Tulbaghia violacea Harv. (Alliaceae) is a small bulbous herb which belongs to the family, Alliaceae, most commonly associated with onions and garlic. In South Africa (SA), this&nbsp / herb has been traditionally used in the treatment of various ailments, including fever, colds, asthma, paralysis, hypertension (HTN) and stomach problems. The aim of this study&nbsp / was to evaluate the effect of methanol leaf extracts (MLE) of T. violacea on the blood pressure (BP) and heart rate (HR) in anaesthetized male spontaneously hypertensive rats / &nbsp / and to find out the mechanism(s) by which it acts. The MLE of T. violacea (5 - 150 mg/kg), angiotensin I (ang I, 3.1 - 100 &mu / g/kg), captopril (10 mg/kg), angiotensin II (ang II, 3.1 - 50&nbsp / g/kg), losartan (30 mg/kg), phenylephrine (0.01 &ndash / 0.16 mg/kg), prazosin (1 mg/kg), dobutamine (0.2 &ndash / 10.0 &mu / g/kg), propranolol (0.1 - 12.8 mg/kg), muscarine (0.16 -10 &mu / g/kg),&nbsp / and atropine (0.02 - 20.48 mg/kg) were administered intravenously into male spontaneously hypertensive rats (SHR) weighing between 300 g and 350 g and aged less than 5&nbsp / months. The MLE of T. violacea and/or the standard drugs were infused alone, simultaneously, or separately into each animal. The BP and HR were measured via a pressure&nbsp / transducer connecting the femoral artery and the Powerlab. The vehicle (0.2 mls of a mixture of dimethylsulfoxide and normal saline), T. violacea (60 mg/kg) and captopril (10&nbsp / mg/kg) were injected intraperitoneally into some SHR for 21 days to investigate the chronic effect of these agents on plasma levels of aldosterone. The mean change, the mean&nbsp / of the individual percentage changes and the percentage difference (in mean) observed with each intervention was calculated and statistically analyzed using the Student&rsquo / s t test&nbsp / for significant difference (p &lt / 0.05). The Microsoft Excel software was used for statistical analysis. T. violacea significantly (p &lt / 0.05) reduced the systolic, diastolic, and mean&nbsp / arterial BP / and HR dose-dependently. In a dose-dependent manner, ang I, ang II, phenylephrine significantly (p &lt / 0.05) increased the BP, while propranolol, muscarine and&nbsp / atropine reduced the BP. The increases in BP due to dobutamine were not dose-dependent. In a dose dependent manner, phenylephrine and propranolol reduced the HR, while dobutamine increased the HR. The effect of ang I, ang II, muscarine and atropine on HR were not dose-dependent / with both increases as well as decreases observed with ang&nbsp / I, and II and atropine, while decreases were seen with muscarine. Captopril produced&nbsp / significant (p &lt / 0.05) reduction in BP which were not associated with any change in HR. The co-infusion of ang I with the MLE produced significant (p &lt / 0.05) reduction in BP, which were not associated with significant changes in HR. The co-infusion of ang II with the&nbsp / MLE did not produce any significant changes in BP or HR when compared to the infusion of the standard drug alone. The co-infusion of phenylephrine with the MLE did not&nbsp / produce any significant change in BP or HR when compared to the values obtained with the infusion of the standard drug alone, in both the absence and presence of prazosin.&nbsp / The co-infusion of dobutamine with T. violacea produced siginificant (p &lt / 0.05) increases in DBP which were associated with significant (p &lt / 0.05) reductions in HR, when&nbsp / compared to the values obtained with the infusion of the standard drug alone. Theco-infusion of atropine with the MLE did not produce any significant change in BP or HR when&nbsp / compared to the values obtained with the infusion of atropine alone. However, the infusion of T. violacea, 20 minutes after pre-treating animals with atropine (5.12 mg/kg) lead to&nbsp / dose dependent significant (p &lt / 0.05) increases in BP, which were associated with dose-dependent increases in HR. The chronic treatment of animals with T. violacea or&nbsp / captropril produced (a) signicant (p &lt / 0.05) reductions in the plasma levels of aldosterone when compared to the values obtained in the vehicle-treated group, (b) produced&nbsp / signifiant (p &lt / 0.05) reduction in BP in the captopril treated group when compared to the vehicle-treated, (c) did not produce any signficant change in BP in the T. violacea-treated&nbsp / group when compared to the vehicle-treated group and (d) did not produce any signifiant change in HR or body weight in any of the groups. The result obtained in this study&nbsp / suggests that T. violacea reduced BP and HR in the SHR. Secondly, the BP and HR reducing effect of the MLE may involve a) the inhibition of the ACE, b) the inhibition of the &beta / 1&nbsp / adrenoceptors, c) the stimulation of the muscarinic receptors and d) the reduction of the levels of aldosternone in plasma. The results also&nbsp / suggest that the MLE may not act&nbsp / through the angiotensin II receptors or the &alpha / 1 adrenergic receptors.&nbsp / </p>

Effect of Tulbaghia violacea on the blood pressure and heart rate in male spontaneously hypertensive wistar rats

Raji, Ismaila

January 2011

Doctor Pharmaceuticae - DPharm / Tulbaghia violacea Harv. (Alliaceae) is a small bulbous herb which belongs to the family, Alliaceae, most commonly associated with onions and garlic. In South Africa (SA), this herb has been traditionally used in the treatment of various ailments, including fever, colds, asthma, paralysis, hypertension (HTN) and stomach problems. The aim of this study was to evaluate the effect of methanol leaf extracts (MLE) of T. violacea on the blood pressure (BP) and heart rate (HR) in anaesthetized male spontaneously hypertensive rats and to find out the mechanism(s) by which it acts. The MLE of T. violacea (5 - 150 mg/kg), angiotensin I (ang I, 3.1 - 100 mg/kg), captopril (10 mg/kg), angiotensin II (ang II, 3.1 - 50 g/kg), losartan (30 mg/kg), phenylephrine (0.01 ; 0.16 mg/kg), prazosin (1 mg/kg), dobutamine (0.2 ; 10.0mg/kg), propranolol (0.1 - 12.8 mg/kg), muscarine (0.16 -10 mg/kg), and atropine (0.02 - 20.48 mg/kg) were administered intravenously into male spontaneously hypertensive rats (SHR) weighing between 300 g and 350 g and aged less than 5; months. The MLE of T. violacea and/or the standard drugs were infused alone, simultaneously, or separately into each animal. The BP and HR were measured via a pressure transducer connecting the femoral artery and the Powerlab. The vehicle (0.2 mls of a mixture of dimethylsulfoxide and normal saline), T. violacea (60 mg/kg) and captopril (10 mg/kg) were injected intraperitoneally into some SHR for 21 days to investigate the chronic effect of these agents on plasma levels of aldosterone. The mean change, the mean of the individual percentage changes and the percentage difference (in mean) observed with each intervention was calculated and statistically analyzed using the Student t test for significant difference (p < 0.05). The Microsoft Excel software was used for statistical analysis. T. violacea significantly (p < 0.05) reduced the systolic, diastolic, and mean arterial BP; and HR dose-dependently. In a dose-dependent manner, ang I, ang II, phenylephrine significantly (p < 0.05) increased the BP, while propranolol, muscarine and atropine reduced the BP. The increases in BP due to dobutamine were not dose-dependent. In a dose dependent manner, phenylephrine and propranolol reduced the HR, while dobutamine increased the HR. The effect of ang I, ang II, muscarine and atropine on HR were not dose-dependent; with both increases as well as decreases observed with ang I, and II and atropine, while decreases were seen with muscarine. Captopril produced significant (p < 0.05) reduction in BP which were not associated with any change in HR. The co-infusion of ang I with the MLE produced significant (p < 0.05) reduction in BP, which were not associated with significant changes in HR. The co-infusion of ang II with the MLE did not produce any significant changes in BP or HR when compared to the infusion of the standard drug alone. The co-infusion of phenylephrine with the MLE did not produce any significant change in BP or HR when compared to the values obtained with the infusion of the standard drug alone, in both the absence and presence of prazosin. The co-infusion of dobutamine with T. violacea produced siginificant (p < 0.05) increases in DBP which were associated with significant (p < 0.05) reductions in HR, when compared to the values obtained with the infusion of the standard drug alone. Theco-infusion of atropine with the MLE did not produce any significant change in BP or HR when compared to the values obtained with the infusion of atropine alone. However, the infusion of T. violacea, 20 minutes after pre-treating animals with atropine (5.12 mg/kg) lead to dose dependent significant (p< 0.05) increases in BP, which were associated with dose-dependent increases in HR. The chronic treatment of animals with T. violacea or captropril produced (a) signicant (p < 0.05) reductions in the plasma levels of aldosterone when compared to the values obtained in the vehicle-treated group, (b) produced signifiant (p< 0.05) reduction in BP in the captopril treated group when compared to the vehicle-treated, (c) did not produce any signficant change in BP in the T. violacea-treated group when compared to the vehicle-treated group and (d) did not produce any signifiant change in HR or body weight in any of the groups. The result obtained in this study suggests that T. violacea reduced BP and HR in the SHR. Secondly, the BP and HR reducing effect of the MLE may involve a) the inhibition of the ACE, b) the inhibition of the beta; adrenoceptors, c) the stimulation of the muscarinic receptors and d) the reduction of the levels of aldosternone in plasma. The results also suggest that the MLE may not act through the angiotensin II receptors or the alpha adrenergic receptors. / South Africa

Tulbaghia violacea

Spontaneously hypertensive rats

Blood pressure

Heart rate

Renin angiotensin aldosterone system

Angiotensin converting enzyme

Angiotensin II receptors

α1 Adrenergic receptors

β1 Adrenergic receptors

Muscarinic receptors

Aldosteron

Treinamento intervalado de alta intensidade promove controle pressórico, melhora a tolerância ao exercício e função cardíaca em ratos espontaneamente hipertensos / High intensity interval training promotes pressure control, and improves tolerance to exercise and heart function in spontaneously hypertensive rats

SOUZA, Francilene Lima Agostinho de

30 October 2017

Submitted by Adriana Martinez (amartinez@unoeste.br) on 2018-02-07T17:06:20Z No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Francilene.pdf: 356698 bytes, checksum: 1dbb03ec82dfb5f6f0997237b2784d9a (MD5) / Made available in DSpace on 2018-02-07T17:06:20Z (GMT). No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Francilene.pdf: 356698 bytes, checksum: 1dbb03ec82dfb5f6f0997237b2784d9a (MD5) Previous issue date: 2017-10-30 / Introduction: Systemic Arterial Hypertension (SAH) is a serious public health problem, especially for the elderly, and can lead to concentric hypertrophy an important risk factor for heart failure, which is considered a predictor of increased cardiovascular morbimortality. Studies have shown that High Intensity Interval Training (HIIT) may also be indicated for hypertensive patients. However, to the authors’ knowledge, no studies have evaluated HIIT in cardiac remodeling of animals with systemic arterial hypertension. Objective: to evaluate in spontaneously hypertensive rats (SHR) submitted to HIIT, pressure control, exercise tolerance and cardiac remodeling. Methods: 20 SHR rats were divided into two groups: sedentary (SHR-SED, n= 9) and HIIT training (SHR-HIIT, n= 11); and Wistar Kyoto rats composed the control group (WKY, n= 6), 12 months of age. The animals were familiarized with HIIT for a week with 10 minutes on the treadmill adapted for rodents. An incremental stress test was performed to exhaustion to adjust exercise intensity. The HIIT was performed five times a week for eight weeks. Before and after HIIT, blood pressure (BP) was measured by plethysmography and a maximal exercise capacity test was performed. Cardiac remodeling was assessed through echocardiography and after euthanasia, the isolated papillary muscle was evaluated. For comparison between groups, we used ANOVA followed by the Tukey test or Kruskal-Wallis and Dunn tests (p <0.05). Results: HIIT decreased the variation (Δ%) of SBP (SHR-SED=Δ% 12.5 vs. SHR-HIIT=Δ% -4.34; p = 0.005), increased the distance traveled, being 82.7% higher in the SHR-HIIT group (SHR-SED=183.0±88.08m; vs. SHR-HIIT=1126.0±187.1m; p<0.001) and reduced the resting tension of the papillary muscle (WKY=0.77 ± 0.216; SHR-SED=1.26 ± 0.20; SHR-HIIT=0.67 ± 0.23; p=0.0001). Conclusion: In SHR rats, HIIT decreased BP variation, improved functional capacity and ameliorated pathological cardiac remodeling. / Introdução: a Hipertensão Arterial Sistêmica (HAS), um grave problema de saúde pública, pode levar à hipertrofia concêntrica – um importante fator de risco para insuficiência cardíaca, que é considerada um preditor de maior morbimortalidade cardiovascular. Estudos evidenciam que o Treinamento Intervalado de Alta Intensidade (HIIT) pode ser indicado para hipertensos. Entretanto, para conhecimento, não há estudos que avaliaram o HIIT na remodelação cardíaca de animais com hipertensão arterial sistêmica. Objetivo: avaliar em ratos espontaneamente hipertensos (SHR) submetidos ao HIIT, o controle pressórico, a tolerância aos exercícios e o remodelamento cardíaco. Métodos: foram utilizados 20 ratos SHR divididos em dois grupos: sedentários (SHR-SED, n=9) e com treinamento HIIT (SHR-HIIT, n=11); e ratos Wistar Kyoto no grupo controle (WKY, n=6), com 12 meses. Os animais foram familiarizados antes do início do teste durante uma semana com 10 minutos, na velocidade de 6 metros por minutos na esteira adaptada para roedores. Realizou-se um teste de esforço incremental, iniciando-se com 10 minutos de aquecimento na velocidade de 6 metros por minutos, sem inclinação até que os ratos chegassem a exaustão, para graduar a intensidade do exercício. O HIIT foi executado cinco vezes por semana, durante oito semanas. Antes e após o HIIT, a pressão arterial (PA) foi aferida por pletismosgrafia e foi realizado um teste de capacidade máxima ao exercício. O remodelamento cardíaco foi avaliado pelo ecocardiograma e, após eutanásia, avaliou-se o músculo papilar isolado. Para comparação entre os grupos foi utilizado ANOVA seguido de Tukey ou Kruskal-Wallis e Dunn’s (p<0.05). Resultados: o HIIT diminuiu a PAS (SHR-SED=Δ%12.05 vs. SHR-HIIT=Δ%-4.34; p=0.005), aumentou a distância percorrida, sendo 82,7% maior no grupo SHR-HIIT (SHR-SED=183.0±88.08m vs. SHR-HIIT=1126.0±187.1m; p<0.0001) e reduziu a tensão de repouso do músculo papilar (WKY=0.77 ± 0.216; SHR-SED=1.26 ± 0.20; SHR-HITT=0.67 ± 0.23; p=0.0001). Conclusão: o HIIT em ratos SHR diminuiu a variação da PA, melhorou a capacidade funcional e amenizou o remodelamento cardíaco patológico.

CIENCIAS AGRARIAS::MEDICINA VETERINARIA

Avaliação do estresse oxidativo e modulação autonômica cardiovascular pós-irradiação de laser de baixa intensidade em ratos espontaneamente hipertensos: estudo experimental

Tomimura, Suely

17 December 2013

Submitted by Nadir Basilio (nadirsb@uninove.br) on 2015-07-20T18:01:54Z No. of bitstreams: 1 Suely Tomimura.pdf: 1781054 bytes, checksum: acaac7dbd088721fbe65530e5cd96c5f (MD5) / Made available in DSpace on 2015-07-20T18:01:54Z (GMT). No. of bitstreams: 1 Suely Tomimura.pdf: 1781054 bytes, checksum: acaac7dbd088721fbe65530e5cd96c5f (MD5) Previous issue date: 2013-12-17 / Due to the increasing numbers of Systemic Arterial Hypertension (HBP) patients in population and its senescence, steadily increased from 600 million in 1980 to 1.2 billion in 2008. The World Health Organization (WHO) in 2009 attributed to high blood pressure (BP) was the death cause for 9.5 million people worldwide. Currently, the hypertension has become a serious public health problem. This entity is an important risk factor for congestive heart failure, cerebrovascular disease, acute myocardial infarction, nephropathy, retinopathy and peripheral vascular insufficiency. Studies have suggested that laser photobiomulation, employing a low power, acts into the inflammatory and proliferative phases of tissue repair, by modulating the inflammatory mediators synthesis as same as the Reactive Oxygen Species (ROS). According scientific publications indicate that the inflammation component is closely related to systemic arterial hypertension as well as possibly to the oxidative stress, both participates in the Hypertension genesis. The aim of this study was to verify the long-term effects of Low Level Laser Therapy (LLLT) application in Spontaneously Hypertensive Rats-SHR (Spontaneously Hypertensive Rats) through on cardiovascular autonomic modulation and oxidative stress in the blood. The experiment consisted in 3 phases: Phase I – LLLT irradiation on SHR: The experiment's phase I consisted of animal’s irradiation, when the laser group received three times LLLT applications weekly for a 7 weeks total; the sham group received three times per week of LLLT simulation for 7 weeks and a total of 21 applications. Prospective, randomized, controlled study, with 16 SHR approximately 2 months age, randomly divided into 2 groups : Sham (n = 8) and Laser (n = 8). The animals were irradiated in a prompt, onto the tail’s dorsal area, using a Diode Laser (MMOptics, São Carlos, SP, Brazil) with a wavelength (λ) of 780 ± 2 (nm), output power at 40 mW, with a 0.04 cm2 beam area, dose of 30 J/cm2 power density of 1W/cm2 and irradiation time of 90 s. In Phase II - Hemodynamic and autonomic cardiovascular evaluation: for a period of 7 weeks, consisted in the cannulation procedure, collecting and analysis. The animals were cannulated, evaluated hemodynamically and analyzed the cardiovascular autonomic modulation. Phase III - Oxidative stress analysis, were analyzed: a) protein damage; b) cell membrane damage; c) antioxidant enzyme activity; d) nitrite concentrations. Data from phase II and III were collected and statistically analyzed applying One Way ANOVA test, followed by post hoc Student - Newman Keulls and considering the significance level of p < 0.05, equivalent to an error α 0.05. The results demonstraded hemodynamic parameters of group LLLT treated showed a BP reduction, when compared with the Sham group. In laser group the diastolic arterial pressure (DAP) showed a reduction of -14 mmHg (± 143 * 4 x 157 ± 3 mmHg Sham) and mean arterial pressure (MAP) - 13mmHg (169 ± 4 * x 182 ± 4 mmHg Sham) there were statistically significant difference. Although the value of systolic arterial pressure (SAP) (196 ± 5 x 207 ± 4 mmHg) showed no differences. There was a decreased in resting HR with a statistically significant difference in the laser group compared to Sham (312 ± 14 vs. 361 ± 13 bpm sham). The spectral reviews in the field of time and frequency showed that the Laser group decreased sympathetic activity on the heart and blood vessels while compared to the Sham group. The heart rate variation was analyzed using the DP-PI ( standard deviation of the pulse interval) VAR-PI components (pulse interval variability) and it demonstrated that LLLT was effective in diminishing variation in heart rate (HR) and sympathetic activity in heart, inducing a substantial fall in blood pressure. Lasertherapy presented a rise in spectral low-frequency component in the pulse interval (LF - IP action of the sympathetic at heart), though the sham group showed up exaggeratedly decreasing (6.77 ± 4:35 and 2:31 ± 0:16 ms ² Sham) as a function of saturation variation. Thus, there was a significant reduction in sympathetic activity after LLLT using. A high-frequency band on interval pulse HF-IP (parasympathetic activity) showed no statistically significant differences between the groups and Laser Sham group. The baroreceptor sensitivity, assessed by the alpha index, signalized a significant increase in the Laser (1:07 ± 0:23 vs. 0:45 ± 0:20 ms / mmHg Sham) group, presenting an improvement in the receptors sensitivity. The baroreflex results were associated with other relevant data, the VAR - SAP (49.55 ± 15.94 * vs 70.51 ± 13:55 mmHg² Sham) and SD -SAP (6.94 ± 1.21 * vs 8.68 ± 1.11 mmHg Sham) that proved to be diminished in the laser group, indicating baroreflex improvement sensitivity concomitantly to the positive SAP variation reduction of. There were no significant differences in baseline SAP (196 ± 5 vs. 207 ± 4 mmHg Sham) between the two groups. The results in the oxidative stress and autonomic analysis demonstrated an association between increased NO production (nitrite 0:36 ± 0:03 vs 0:26 ± 0:03 nm / mg Sham) and decreased in the vascular sympathetic (LF - SAP 7.28 ± 1.63 * vs 9.86 ± 0.47 Sham), both leading to a profound vasodilatation then a significant fall in of blood pressure. Lasertherapy shown to alter the plasma parameters such as oxidative nitrite, revealing an NO increased metabolism, as described above and, moreover, accounted for a significant reduction in carbonyl plasma concentration (vs 3.93 ± 0.24, 4.75 ± 0:26 * nm / mg Sham). Our experimental study indicate that LLLT was able to reduce the oxidative stress parameters through diminishing the damage to the proteins. The enzymatic defense was analyzed by the enzyme SOD concentration in blood plasma, denoted that no significant differences (4:42 ± 0:10 4:25 ± 0:06 vs usod / mg) between groups. Thus, low level laser therapy has shown to improve cardiovascular autonomic activity as well as oxidative parameters which resulted in steadily staggeringly reduce the blood pressure of hypertensive animals. / Em razão do aumento populacional e a senescência, o número de indivíduos com Hipertensão Arterial Sistêmica (HAS) cresceu de 600 milhões em 1980 para 1,2 bilhões (OMS 2011). Lim (2012) atribuiu que a pressão arterial (PA) elevada fosse a causa mortis de 9,5 milhões de indivíduos ao redor do mundo. Atualmente, a HAS tornou-se um grave problema de saúde pública. A hipertensão é um importante fator de risco para insuficiência cardíaca congestiva, doenças cerebrovasculares, infarto agudo do miocárdio, nefropatia, insuficiência vascular periférica e retinopatia hipertensiva. Considerando publicações científicas que demonstram que o componente da inflamação e do estresse oxidativo estão intimamente relacionados à gênese da hipertensão arterial sistêmica (HAS), e que o laser com potência baixa tem efeito positivo no estresse oxidativo e apresenta ação antiinflamatória eficaz, desta forma buscamos estudar a resposta da Laserterapia na HAS. Inúmeros estudos vêm sugerindo, ao longo de décadas, que a fotobiomulação pelo laser empregado uma potência baixa, atua durante as fases inflamatórias e proliferativas da reparação tissular, modulando síntese de mediadores inflamatórios e espécies reativas de oxigênio (ROS). O objetivo deste estudo foi analisar os efeitos da aplicação do laser de baixa intensidade em ratos espontaneamente hipertensos SHR (Spontaneously Hypertensive Rats) em longo prazo na modulação autonômica cardiovascular e no estresse oxidativo sangúineo. Estudo prospectivo, randomizado e controlado com 16 ratos SHR, divididos aleatoriamente em 2 grupos: Sham (n=8) e Laser (n=8).O experimento foi dividido em três fases: Fase I – Irradiação dos animais: constituiu-se na irradiação com laser nos animais SHR, onde o grupo Laser recebeu três aplicações semanais de LBI durante sete semanas; já no grupo Sham foram realizados três simulações de aplicação semanais de Laser de Baixa Intensidade (LBI) durante 7 semanas, totalizando 21 aplicações de LBI. Os animais foram irradiados pontualmente, na região dorsal da cauda, utilizando um Laser Diodo (MMOptics, São Carlos, SP, Brasil) com comprimento de onda de λ = 780 ± 2 (nm); potência de 40 mW, área do feixe de 0,04 cm2, densidade de energia de 30 J/cm2, densidade de potência de 1W/cm2, tempo total de irradiação de 90 s de exposição. Fase II – Avaliação hemodinâmica e autonômica cardiovascular: constituiu-se nos procedimento de canulação, registro de dados e coleta de material, teve inicio após sete semanas de irradiação. Os animais canulados foram avalidados de forma hemodinâmica, bem como analisada a modulação autonômica cardiovascular. Fase III – Análises do estresse oxidativo, foram analisadas: a) danos à proteína; b) danos à membrana celular; c) atividade enzimática; d) concentração de nitrito. Os dados da fase II e III foram coletados e analisados estatisticamente através dos testes Anova One Way, seguido de Post Hoc de Student Newman-Keulls, considerando-se o nível de significância p < 0,05, equivalendo a um erro α de 0.05. Os resultados hemodinâmicos do grupo tratado com LLLT denotaram um decréscimo significativo da PA quando comparado com o grupo Sham. A pressão arterial diastólica (PAD) do grupo Laser revelou uma redução de -14 mmHg (143± 4*vs157±3 mmHg Sham) e a pressão arterial média (PAM) -13mmHg (169±4*vs182±4 mmHg Sham), a frequência cardíaca (FC) em repouso (312±14*vs361±13 bpm Sham) revelando uma diferença estatisticamente significante, porém o valor da pressão arterial sistólica(PAS) não mostrou (196±5 x 207±4 mmHg) alterações entre os grupos. As avaliações espectrais no domínio do tempo e da frequencia demostraram que o grupo Laser reduziu a atividade simpática sobre o coração e vasos sanguíneos quando comparados ao grupo Sham. A variação frequência cardíaca foi analisada através dos componentes VAR-IP (variabilidade do intervalo de pulso) e o DP-IP (desvio do intervalo de pulso) que evidenciaram que o LBI foi eficaz no decréscimo variação da FC e da atividade simpática no coração, induzindo assim a queda das pressões arteriais. A laserterapia mostrou um incremento no componente espectral baixa frequência no intervalo de pulso (BF-IP ação do simpático no coração), porém o grupo Sham apresentou-se exacerbadamente diminuído (6.77 ± 4.35 e 2.31±0.16 ms² Sham) em função da saturação da variação desse componente que foi reduzido. Desta forma, houve um importante decréscimo da atividade simpática com o uso do LBI, significando uma importante diminuição dos níveis pressóricos. A banda de alta frequência (AF-IP atividade parassimpática cardíaca) não mostrou diferenças estatísticas significantes entre os grupos Laser e grupo Sham. A sensibilidade dos barorreceptores, avaliada pelo índice alfa, demonstrou um significativo incremento da resposta no grupo Laser (1.07 ± 0.23 vs 0.45 ± 0.20 ms/mmHg Sham), revelando uma melhora na sensibilidade destes receptores. Os resultados dos barorreflexos encontravam-se associados a outro dado relevante, o componente VAR-PAS (49.55 ± 15.94* vs 70.51 ± 13.55 mmHg² Sham) e DP-PAS (6.94 ± 1.21* vs 8.68 ± 1.11 mmHg Sham) que mostrou-se diminuído no grupo Laser, indicando que a melhora da sensibilidade barorreflexa ocorreu, concomitantemente, à redução positiva da variação da PAS. Não houve diferenças estatísticas significantes na PAS basal (196±5 vs 207 ± 4 mmHg Sham) entre os dois grupos. Já os resultados encontrados na análise do estresse oxidativo e autonômica demonstraram uma associação entre o incremento da produção do óxido nitrico (NO) (nitrito 0.36 ± 0.03 vs 0.26 ± 0.03 nm/mg Sham) e redução do simpático vascular (BF-PAS 7.28 ± 1.63* vs 9.86 ± 0.47 Sham), ambos levando a uma vasodilatação com consequente queda dos níveis pressóricos arteriais. A laserterapia mostrou alterar parâmetros oxidativos como as espécies reativas de nitrogênio (RNS reactive nitrogen species), o nitrito plasmático, revelando um aumento do metabolismo do NO, como já descrito anteriormente e denotou uma diminuição significativa da concentração de carbonilas plasmáticas (3.93 ± 0.24 * vs 4.75 ± 0.26 nm/mg Sham). A defesa enzimática foi analisada através da concentração da enzima SOD no plasma sanguíneo, que não apontou diferenças significativas (4.42 ± 0.10 vs 4.25 ± 0.06 usod/mg) entre os grupos. Evidenciamos que o LBI foi capaz de reduzir este parâmetro oxidativo, reduzindo os danos às proteínas decorrente do estresse. Desta forma, concluímos que a laserterapia demonstrou resposta positiva ao melhorar a atividade autonômica cardiovascular e parâmetros oxidativos que resultaram na redução dos níveis pressóricos dos animais hipertensos.

laser de baixa intensidade (lllt)

laserterapia

hipertensão

modulação autonômica cardiovascular

disfunção endotelial

estresse oxidativo

espécies reativas de oxigênio (eros)

alterações hemodinâmicas

shr (ratos espontaneamente hipertensos)

low level laser therapy (lllt)

lasertherapy

hypertension

cardiovascular autonomic modulation

oxidative stress

reactive oxygen species (ros)

endothelial inflammation

spontaneously hypertensive rats (shr)

hemodynamic response

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