Evidence Linking Alterations in the Moment-to-Moment Pressure-Natriuresis Mechanism to Hypertension and Salt-Sensitivity in Rodents

Komolova, Marina

13 May 2010

Hypertension and salt-sensitivity are independent risk factors for cardiovascular disease. Although both conditions are idiopathic, they develop due to a complex interplay between susceptibility genes and environmental factors. Given that the kidney plays an important role in regulating blood pressure, in particular, by maintaining sodium and water balance via pressure-natriuresis, it is not surprising that disturbances in the proper functioning of this intrarenal mechanism have been linked to these conditions. Although direct coupling of changes in renal arterial pressure (RAP) to renal interstitial hydrostatic pressure (RIHP) and consequent sodium excretion is well established, few studies have characterized the moment-to-moment aspects of this process. Thus, the main focus of the research presented herein was to characterize the moment-to-moment RAP-RIHP relationship, and assess the functioning of this intrarenal mechanism in various animal models of genetic and environmentally-induced hypertension and/or salt-sensitivity. In adult normotensive rats, the response time of RIHP to acute changes in RAP was rapid (<2 seconds), and the moment-to-moment RAP-RIHP relationship was linear over a wide range of pressures. Additionally, the functioning of this relationship was not affected by inhibition of the renin-angiotensin system and autonomic nervous system. Further, the acute RAP-RIHP relationship was impaired in hypertension and/or salt-sensitivity. Specifically, animals with a hypertensive phenotype (i.e. young spontaneously hypertensive rats [SHR] and pro-atrial natriuretic peptide gene-disrupted mice [ANP -/-]) displayed a rightward shift in the moment-to-moment pressure-natriuresis curve towards higher RAP. This rightward shift was associated with increased structurally-based vascular resistance properties in the hindlimb of young SHR versus their normotensive controls. Salt-sensitive phenotypes were associated with a blunting of this acute mechanism. Specifically, this blunting was evident in both the ANP -/-, a transgenic model of salt-sensitive hypertension, and in adult perinatal iron deficient (PID) rats, a developmentally programmed model of salt-sensitivity. It appears that a blunting in the RAP-RIHP relationship is influenced by an imbalance of key blood pressure modulating factors (e.g. ANP). Further, visceral obesity was associated with salt-sensitivity in PID rats; however the mechanism(s) are yet to be elucidated. Novel methodologies (MRI, abdominal girth) were developed for non-invasive assessment of visceral obesity to aid future research. / Thesis (Ph.D, Pharmacology & Toxicology) -- Queen's University, 2010-05-12 10:11:21.197

pressure-natriuresis

arterial pressure

renal interstitial hydrostatic pressure

renal arterial pressure

hypertension

salt-sensitivity

animal models

genetic

environmental

fetal programming

visceral adipose tissue

magnetic resonance imaging

abdominal girth

La néoglucogenèse rénale : un nouvel aspect dans la restriction de croissance intra-utérine chez le rat

Khoury, Etienne

06 1900

Bien que l’environnement intra-utérin défavorable soit associé à des conditions pathologiques à l’âge adulte, les mécanismes mis en place in utero ne sont pas encore élucidés. Nous avons établi un modèle de restriction de croissance intra-utérine (RCIU) en donnant une diète faible en sodium à la rate pendant la dernière semaine de gestation. Ce modèle se caractérise par une diminution de perfusion placentaire et une redistribution du flot sanguin, favorisant l’irrigation des organes nobles (cœur et cerveau) au détriment du rein fœtal. De plus, l’expression rénale du facteur de croissance endothéliale vasculaire (VEGF) est diminuée chez le fœtus. L’hypothèse de travail est que la néoglucogenèse hépatique et rénale augmente chez les fœtus RCIU afin de compenser la diminution de perfusion placentaire, et que l’expression rénale des récepteurs de VEGF (Flt-1 et Flk-1) est altérée à la suite de la redistribution du flot sanguin. Nos objectifs étaient de comparer l’expression protéique des enzymes de la néoglucogenèse et des récepteurs de VEGF entre les fœtus témoins et RCIU. L’aldolase B, la fructose-1,6-biphosphatase et la glucose-6-phosphatase augmentent dans les reins de fœtus RCIU par rapport aux témoins alors qu’aucun changement n’est observé dans le foie. De plus, l’expression de ces enzymes est différente selon le sexe du fœtus. Une diminution de Flt-1 est notée dans les reins de fœtus RCIU. Nos résultats démontrent que des adaptations surviennent chez le fœtus à la suite d’une insulte intra-utérine favorisant sa survie mais ayant des conséquences telles que la dysfonction rénale observée chez les adultes de ce modèle animal. À long terme, ces travaux pourront permettre d’entrevoir des avenues pour mieux identifier les approches de prévention lors de naissance à la suite d’une RCIU. / An adverse intrauterine environment is associated with several pathological conditions at adult age, however, the mechanisms underlying such a link remain to be elucidated. Feeding a low-sodium diet to dams during the last week of gestation consistently resulted in giving birth to intrauterine growth restriction (IUGR) offsprings. The present model is characterized by a reduced placental perfusion and a redistribution of a preferential blood flow to the brain and heart at the expense of the kidney. Moreover, renal expression of the vascular endothelial growth factor (VEGF) is decreased in the IUGR fetuses. In this view, we hypothesize that the hepatic and renal gluconeogenesis is increased in the IUGR fetus in order to compensate the diminished placental perfusion, and the renal expression of VEGF receptors (Flt-1 and Flk-1) is altered in response to the redistribution of the blood flow. The specific aim of this study was to compare the protein expression of gluconeogenic enzymes and VEGF receptors between IUGR and control fetuses. Aldolase B, fructose-1,6- biphosphatase and glucose-6-phosphatase were significantly increased in the IUGR fetal kidneys compared to controls. However, gluconeogenic enzymes did not show any significant change in the IUGR liver. The fetal sex had an impact on the enzymes expression. A decreased expression of Flt-1 was also noted in the kidneys of the IUGR fetuses. Our results pointed out alterations in the fetal life that may be, in a way, essentiel for the survival of the fetus, but somehow, responsible for many pathological consequences at adult age, as the renal dysfunction observed in the present model. For the long term, this work may lead to many future perspectives helping to prevent several diseases, such as hypertension or diabetes for an IUGR case.

Programmation fœtale

Métabolisme

Glucose

Fetal programming

Metabolism

Glucose

Vascular Endothelial Growth Factor

Administração crônica de cafeína durante a gestação afeta o remodelamento cardíaco e expressão dos componentes do sistema renina angiotensina da prole adulta de camundongos C57BL/6 / Chronic administration of caffeine during gestation affects cardiac remodeling and expression of renin angiotensin system components in adult C57BL/6 mice offspring

Diana de Freitas Serapião Moraes

30 July 2012

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Este estudo teve como objetivo avaliar o papel da administração crônica de cafeína durante a gestação de camundongos C57BL/6 sobre o remodelamento cardíaco e a expressão de componentes do sistema renina-angiotensina (SRA) na prole macho adulta. Fêmeas C57BL/6 grávidas foram divididas em dois grupos (n = 10): grupo controle (C), progenitoras foram injetadas apenas com o veículo (solução salina NaCl 0,9%), e grupo cafeína (CF), progenitoras receberam diariamente uma injecção subcutânea contendo 20 mg/kg de cafeína (1 mg/ml de solução salina). Após o desmame, os filhotes tiveram livre acesso à ração padrão até 90 dias de idade quando foram sacrificados. Rim e ventrículo esquerdo (VE) foram coletados para análise estrutural e western blotting. O grupo cafeína mostrou uma redução significativa no ganho de massa corporal (MC) (-18%; P <0,0001). O grupo cafeína apresentou ainda um aumento da pressão arterial sistólica (+ 48%; P <0,0001) e freqüência cardíaca (+10%; P <0,01) em relação ao grupo controle. A massa do VE corrigida pela MC no grupo da cafeína foi maior que no grupo C (+10%; P <0,01). O grupo cafeína apresentou um aumento na área de cardiomiócitos (+40%; P <0,05), e reduzida densidade capilar (-25%; P <0,05). No rim, as expressões de renina (128%; P <0,05) e dos receptores 1 da angiotensina II (AT1R) (88%; P <0,05) foram significativamente maiores nos animais do grupo cafeína. No VE, o grupo cafeína demonstrou aumento da expressão de ECA (+30%; P <0,05), angiotensina II (+60%; P <0,01), e AT1R (+77%; P <0,01) e diminuição da expressão do receptor 2 de angiotensina II (-46%; P <0,05). Em conclusão, a administração crônica de cafeína durante a gestação, possivelmente programa a expressão de componentes de sistema renina-angiotensina, levando à ativação persistente do SRA renal e cardíaco local, que por sua vez promove o aumento da pressão sanguínea, remodelação e efeitos cardíacos adversos. / This study aimed to evaluate the role of caffeine chronic administration during gestation of C57BL/6 mice on cardiac remodeling and the expression of components of the renin-angiotensin system (RAS) in male offspring as adults. Pregnant C57BL/6 female mice were divided into two groups (n=10): Control group (C), dams were injected with the vehicle only (saline 0.9% NaCl), and Caffeine group (CF), dams received daily a subcutaneous injection containing 20 mg/kg of caffeine/day (1 mg/ml saline). After weaning, pups had free access to the standard chow until 90 days of age when they were killed. Kidney and left ventricle (LV) were collected for structural analysis and Western blot. Caffeine group showed a significant reduction in body mass (BM) gain (-18%;P<0.0001). Caffeine group had increased systolic blood pressure (+ 48%;P<0.0001) and higher heart rate (+10%;P<0.01) than control group. LV mass adjusted by BM in caffeine group was greater than in C group (+10%;P<0.01). Caffeine group had increase in the area of cardiomyocytes (+40%;P<0.05), and reduced capillary density (-25%;P<0.05). In the kidney, the expressions of renin (+128%; P<0.05) and angiotensin II receptor 1(AT1R) (+88%;P<0.05) were significantly greater in caffeine mice. In the LV, caffeine group showed increased expression of ACE (+30%; P <0.05), angiotensin II (+60%;P<0.01), and AT1R (+77%;P<0.01), and decreased expression of angiotensin II receptor 2 (-46%;P<0.05). In conclusion, chronic administration of caffeine during gestation possibly programs the expression of renin-angiotensin system components, leading to persistent activation of local renal and cardiac RAS, which in turn promotes increased BP and adverse cardiac remodeling.

Camundongo C57BL/6

Cafeína

Programação fetal

Remodelamento cardíaco

Sistema renina-angiotensina

C57BL/6 mice

Caffeine

Fetal programming

Cardiac remodeling

Renin-angiotensin system

MORFOLOGIA

Influência do hipotireoidismo gestacional experimental em sistemas biológicos centrais de regulação da nocicepção em ratos

Alves, Iura Gonzalez Nogueira

29 July 2016

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / Changes in maternal thyroid hormones concentrations during pregnancy can affect the body development of pups. However, despite the recent race for the understanding of the mechanisms that explain the impact of perinatal life in the occurrence of different diseases, little has been done to investigate the role of maternal thyroid hormones for proper development of CNS structures, important in regulating perception nociceptive. In this sense, in the present study we investigate the effect of experimental gestational hypothyroidism (EGH) in biological systems of nociceptive circuitry. The EGH was induced by methimazole to 0.02% in drinking water from ninth day of gestation until delivery. The threshold for noxious temperature was evaluated by using the hot plate apparatus (52 ± 0.2 ° C) in male offspring from methimazole treated dams (OMTD) and offspring from water treated dams (OWTD), on postnatal day (PND) 60 days, in baseline condiction and after a drug injection (morphine, memantine, sertraline and AMPT). In addition, thyroid status was evaluated through the determination of total T3 and T4 serum levels on PND 60, sections through the vlPAG were processed for TH immunofluorescence, the contents of glutamate in the cerebrospinal fluid was measured and evaluated oxidative parameters in spinal cord. The results were expressed mean ± Standard Error values. Three and two way ANOVA, Student t test, Mann-Whitney and correlation test were used. The threshold of statistical significance was set at p<0.05. Thus, our data showed that EGH does not generate significant impact on the treated mothers when they are compared to control, but in the offspring important effects of lack of maternal THs in the intrauterine period were observed. OMTD had less body weight after 60 DPN (p <0.01), higher serum concentration of TT3 (p <0.05), higher analgesia on the hot plate after i.p. morphine, at times 30 and 60 minutes (time factor interaction and treatment (F (4, 80) = 2.50, p <0.05) and increased lipid peroxidation (assessed by quantification of TBARS) in the spinal cord (p <0.01 ). Given the above, we conclude that the lack of THs during pregnancy causes changes in body weight and serum concentrations of T3, as well as in biological systems of nociceptive circuitry. / Alterações das concentrações de hormônios tireoideanos maternos durante a gestação podem afetar o adequado desenvolvimento dos filhotes. No entanto, apesar da corrida recente pela compreensão dos mecanismos que expliquem as repercussões da vida perinatal na ocorrência de distintas doenças, pouco se tem feito para investigar o papel dos hormônios tireoideanos maternos para o adequado desenvolvimento das estruturas do SNC, importantes na regulação da percepção nociceptiva. Nesse sentido, no presente estudo, procurou-se investigar as repercussões do hipotireoidismo gestacional (HGE) materno nos sistemas biológicos centrais de controle nociceptivo. O HGE foi induzido adicionando metimazol a 0,02% na água de beber a partir do nono dia de gestação até o parto. Os machos da prole de mães hipotireoideas (PMH) e eutireoideas (PME) foram submetidos à avaliação basal e após a injeção de drogas (morfina, memantina, sertralina e AMPT), do limiar nociceptivo com 60 dias pós-natal (DPN) por meio do aparato da placa quente (52±0,2 C). Ademais, foi realizada a dosagem da triiodotironina e tiroxina totais (TT3 e TT4, respectivamente) séricos, quantificação de neurônios da substância cinzenta periaquedutal porção ventrolateral (PAGvl) imunomarcados para tirosina hidroxilase, quantificação de glutamato no líquor, além da avaliação de parâmetros oxidativos. Os resultados obtidos foram expressos em valores de média ± erro padrão da média. Para comparação dos dados entre os grupos foi realizado ANOVA three e two-way de medidas repetidas, student t test, Mann-withney e ANCOVA com distância percorrida como co-. O nível crítico fixado foi de 5% (P<0,05). Após análise dos dados foi possível observar que a PMH apresenta menor massa corporal aos 60 DPN (p<0.01), maior concentração sérica de TT3 (p<0.05), maior analgesia na placa quente após a administração i.p. de morfina nos tempos 30 e 60 minutos (fator interação tempo e tratamento (F(4, 80) = 2,50; p <0,05) e maior peroxidação lipídica (avaliada pela quantificação do TBARS) na medula espinhal (p<0.01) quando comparada ao grupo controle. Diante do exposto, concluímos que o HGE não gera repercussões importantes nas mães tratadas, quando estas são comparadas as controle, no entanto, a prole sofre importantes efeitos da carência dos hormônios tireoideanos maternos no período intraútero. A carência de HTs no período gestacional acarreta alterações no peso corporal e nas concentrações séricas de TT3, bem como nos sistemas biológicos de controle nociceptivo.

Ciências da saúde

Hipotireoidismo gestacional

Nocicepção

PAG

Prole

Programação fetal

Estresse oxidativo

Gestational hypothyroidism

Nociception

Rats

Offspring

Fetal programming

Oxidative stress

CIENCIAS DA SAUDE

Administração crônica de cafeína durante a gestação afeta o remodelamento cardíaco e expressão dos componentes do sistema renina angiotensina da prole adulta de camundongos C57BL/6 / Chronic administration of caffeine during gestation affects cardiac remodeling and expression of renin angiotensin system components in adult C57BL/6 mice offspring

Diana de Freitas Serapião Moraes

30 July 2012

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Este estudo teve como objetivo avaliar o papel da administração crônica de cafeína durante a gestação de camundongos C57BL/6 sobre o remodelamento cardíaco e a expressão de componentes do sistema renina-angiotensina (SRA) na prole macho adulta. Fêmeas C57BL/6 grávidas foram divididas em dois grupos (n = 10): grupo controle (C), progenitoras foram injetadas apenas com o veículo (solução salina NaCl 0,9%), e grupo cafeína (CF), progenitoras receberam diariamente uma injecção subcutânea contendo 20 mg/kg de cafeína (1 mg/ml de solução salina). Após o desmame, os filhotes tiveram livre acesso à ração padrão até 90 dias de idade quando foram sacrificados. Rim e ventrículo esquerdo (VE) foram coletados para análise estrutural e western blotting. O grupo cafeína mostrou uma redução significativa no ganho de massa corporal (MC) (-18%; P <0,0001). O grupo cafeína apresentou ainda um aumento da pressão arterial sistólica (+ 48%; P <0,0001) e freqüência cardíaca (+10%; P <0,01) em relação ao grupo controle. A massa do VE corrigida pela MC no grupo da cafeína foi maior que no grupo C (+10%; P <0,01). O grupo cafeína apresentou um aumento na área de cardiomiócitos (+40%; P <0,05), e reduzida densidade capilar (-25%; P <0,05). No rim, as expressões de renina (128%; P <0,05) e dos receptores 1 da angiotensina II (AT1R) (88%; P <0,05) foram significativamente maiores nos animais do grupo cafeína. No VE, o grupo cafeína demonstrou aumento da expressão de ECA (+30%; P <0,05), angiotensina II (+60%; P <0,01), e AT1R (+77%; P <0,01) e diminuição da expressão do receptor 2 de angiotensina II (-46%; P <0,05). Em conclusão, a administração crônica de cafeína durante a gestação, possivelmente programa a expressão de componentes de sistema renina-angiotensina, levando à ativação persistente do SRA renal e cardíaco local, que por sua vez promove o aumento da pressão sanguínea, remodelação e efeitos cardíacos adversos. / This study aimed to evaluate the role of caffeine chronic administration during gestation of C57BL/6 mice on cardiac remodeling and the expression of components of the renin-angiotensin system (RAS) in male offspring as adults. Pregnant C57BL/6 female mice were divided into two groups (n=10): Control group (C), dams were injected with the vehicle only (saline 0.9% NaCl), and Caffeine group (CF), dams received daily a subcutaneous injection containing 20 mg/kg of caffeine/day (1 mg/ml saline). After weaning, pups had free access to the standard chow until 90 days of age when they were killed. Kidney and left ventricle (LV) were collected for structural analysis and Western blot. Caffeine group showed a significant reduction in body mass (BM) gain (-18%;P<0.0001). Caffeine group had increased systolic blood pressure (+ 48%;P<0.0001) and higher heart rate (+10%;P<0.01) than control group. LV mass adjusted by BM in caffeine group was greater than in C group (+10%;P<0.01). Caffeine group had increase in the area of cardiomyocytes (+40%;P<0.05), and reduced capillary density (-25%;P<0.05). In the kidney, the expressions of renin (+128%; P<0.05) and angiotensin II receptor 1(AT1R) (+88%;P<0.05) were significantly greater in caffeine mice. In the LV, caffeine group showed increased expression of ACE (+30%; P <0.05), angiotensin II (+60%;P<0.01), and AT1R (+77%;P<0.01), and decreased expression of angiotensin II receptor 2 (-46%;P<0.05). In conclusion, chronic administration of caffeine during gestation possibly programs the expression of renin-angiotensin system components, leading to persistent activation of local renal and cardiac RAS, which in turn promotes increased BP and adverse cardiac remodeling.

Camundongo C57BL/6

Cafeína

Programação fetal

Remodelamento cardíaco

Sistema renina-angiotensina

C57BL/6 mice

Caffeine

Fetal programming

Cardiac remodeling

Renin-angiotensin system

MORFOLOGIA

Influência do hipotireoidismo gestacional experimental em sistemas biológicos centrais de regulação da nocicepção em ratos

Alves, Iura Gonzalez Nogueira

29 July 2016

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / Changes in maternal thyroid hormones concentrations during pregnancy can affect the body development of pups. However, despite the recent race for the understanding of the mechanisms that explain the impact of perinatal life in the occurrence of different diseases, little has been done to investigate the role of maternal thyroid hormones for proper development of CNS structures, important in regulating perception nociceptive. In this sense, in the present study we investigate the effect of experimental gestational hypothyroidism (EGH) in biological systems of nociceptive circuitry. The EGH was induced by methimazole to 0.02% in drinking water from ninth day of gestation until delivery. The threshold for noxious temperature was evaluated by using the hot plate apparatus (52 ± 0.2 ° C) in male offspring from methimazole treated dams (OMTD) and offspring from water treated dams (OWTD), on postnatal day (PND) 60 days, in baseline condiction and after a drug injection (morphine, memantine, sertraline and AMPT). In addition, thyroid status was evaluated through the determination of total T3 and T4 serum levels on PND 60, sections through the vlPAG were processed for TH immunofluorescence, the contents of glutamate in the cerebrospinal fluid was measured and evaluated oxidative parameters in spinal cord. The results were expressed mean ± Standard Error values. Three and two way ANOVA, Student t test, Mann-Whitney and correlation test were used. The threshold of statistical significance was set at p<0.05. Thus, our data showed that EGH does not generate significant impact on the treated mothers when they are compared to control, but in the offspring important effects of lack of maternal THs in the intrauterine period were observed. OMTD had less body weight after 60 DPN (p <0.01), higher serum concentration of TT3 (p <0.05), higher analgesia on the hot plate after i.p. morphine, at times 30 and 60 minutes (time factor interaction and treatment (F (4, 80) = 2.50, p <0.05) and increased lipid peroxidation (assessed by quantification of TBARS) in the spinal cord (p <0.01 ). Given the above, we conclude that the lack of THs during pregnancy causes changes in body weight and serum concentrations of T3, as well as in biological systems of nociceptive circuitry. / Alterações das concentrações de hormônios tireoideanos maternos durante a gestação podem afetar o adequado desenvolvimento dos filhotes. No entanto, apesar da corrida recente pela compreensão dos mecanismos que expliquem as repercussões da vida perinatal na ocorrência de distintas doenças, pouco se tem feito para investigar o papel dos hormônios tireoideanos maternos para o adequado desenvolvimento das estruturas do SNC, importantes na regulação da percepção nociceptiva. Nesse sentido, no presente estudo, procurou-se investigar as repercussões do hipotireoidismo gestacional (HGE) materno nos sistemas biológicos centrais de controle nociceptivo. O HGE foi induzido adicionando metimazol a 0,02% na água de beber a partir do nono dia de gestação até o parto. Os machos da prole de mães hipotireoideas (PMH) e eutireoideas (PME) foram submetidos à avaliação basal e após a injeção de drogas (morfina, memantina, sertralina e AMPT), do limiar nociceptivo com 60 dias pós-natal (DPN) por meio do aparato da placa quente (52±0,2 C). Ademais, foi realizada a dosagem da triiodotironina e tiroxina totais (TT3 e TT4, respectivamente) séricos, quantificação de neurônios da substância cinzenta periaquedutal porção ventrolateral (PAGvl) imunomarcados para tirosina hidroxilase, quantificação de glutamato no líquor, além da avaliação de parâmetros oxidativos. Os resultados obtidos foram expressos em valores de média ± erro padrão da média. Para comparação dos dados entre os grupos foi realizado ANOVA three e two-way de medidas repetidas, student t test, Mann-withney e ANCOVA com distância percorrida como co-. O nível crítico fixado foi de 5% (P<0,05). Após análise dos dados foi possível observar que a PMH apresenta menor massa corporal aos 60 DPN (p<0.01), maior concentração sérica de TT3 (p<0.05), maior analgesia na placa quente após a administração i.p. de morfina nos tempos 30 e 60 minutos (fator interação tempo e tratamento (F(4, 80) = 2,50; p <0,05) e maior peroxidação lipídica (avaliada pela quantificação do TBARS) na medula espinhal (p<0.01) quando comparada ao grupo controle. Diante do exposto, concluímos que o HGE não gera repercussões importantes nas mães tratadas, quando estas são comparadas as controle, no entanto, a prole sofre importantes efeitos da carência dos hormônios tireoideanos maternos no período intraútero. A carência de HTs no período gestacional acarreta alterações no peso corporal e nas concentrações séricas de TT3, bem como nos sistemas biológicos de controle nociceptivo.

Ciências da saúde

Hipotireoidismo gestacional

Nocicepção

PAG

Prole

Programação fetal

Estresse oxidativo

Gestational hypothyroidism

Nociception

Rats

Offspring

Fetal programming

Oxidative stress

CIENCIAS DA SAUDE

Avaliação do envolvimento do sistema renina-angiotensina nas alterações cardíacas dos machos da prole de ratas Wistar alimentadas com dieta hipossódica, normossódica e hipersódica durante a gestação / Evaluation of the involvement of the renin-angiotensin system on cardiac alterations in male offspring from dams fed a low-, normal- or high-salt diet during pregnancy

Edson Nogueira Alves Rodrigues Junior

27 July 2011

O objetivo do presente estudo consiste em avaliar o efeito da restrição ou sobrecarga de cloreto de sódio (NaCl) durante a gestação sobre a programação de possíveis alterações cardíacas nos machos da prole adulta e sua interação com o sistema renina-angiotensina miocárdico. Ratas Wistar foram alimentadas com dieta hipossódica (HO, 0,15%), normossódica (NR, 1,3%) ou hipersódica (HR2, 8% de NaCl) durante a gestação. Durante a lactação todas as mães receberam dieta NR, assim como as proles desde o desmame até a 20ª semana de idade. Ecocardiograma foi realizado na 20ª semana de idade não sendo constatada nenhuma diferença entre os grupos. Em seguida, metade das proles de cada grupo experimental recebeu uma sobrecarga crônica de cloreto de sódio na dieta na tentativa de revelar diferenças entre grupos, uma vez que a dieta hipersódica é comprovadamente um causador de hipertrofia cardíaca independente dos níveis de pressão arterial. Metade das proles de cada grupo passou a receber dieta hipersódica (hr, 4% de NaCl) da 21ª até a 36ª semana de idade (HOhr, NRhr, HRhr) e as proles restantes foram mantidas em dieta NR (HOnr, NRnr e HRnr) pelo mesmo período. Novo ecocardiograma foi realizado na 30ª semana de idade. Na 36ª semana de idade foi aferida a pressão arterial média e posteriormente os animais foram sacrificados para coleta do ventrículo esquerdo para análise histológica e expressão gênica e protéica dos componentes do sistema renina-angiotensina. As proles de mães alimentadas com dieta hipo ou hipersódica não apresentaram alterações estruturais ou funcionais cardíacas até a 36ª semana de idade, quando mantidas em dieta normossódica. Contudo, as proles HRhr apresentaram hipertrofia concêntrica do ventrículo esquerdo não acompanhada de fibrose, independente da pressão arterial e dos níveis de angiotensina II miocárdica. Surpreendentemente as proles HOhr apresentaram menor pressão arterial quando comparadas com as proles HRhr, NRhr e HOnr. Embora as proles de mães alimentadas com dieta hipossódica durante a gestação não tenham apresentado alterações sugestivas de hipertrofia cardíaca, mesmo após sobrecarga crônica de sal na idade adulta, estas apresentaram menor débito cardíaco após sobrecarga crônica de sal na dieta quando comparadas com as proles HRhr e NRhr e maior número de núcleos por cardiomiócito quando comparadas com proles HOnr. / The aim of the present study was to evaluate the effects of a low or high salt diet during pregnancy on the left ventricle of adult male offspring and its interaction with the cardiac renin-angiotensin system. Low- (LS, 0.15%), normal- (NS, 1.3%) or high-salt (HS, 8% NaCl) diet was given to Wistar rats during pregnancy. During lactation all dams received NS as well as the offspring after weaning. Echocardiogram was done at 20 weeks of age. No differences were observed. In an attempt to stimulate differences between groups, 50% of each offspring group was fed a high-salt (hs, 4% NaCl) diet from the 21st to the 36th week of age (LShs, NShs, HShs). The remaining 50% was maintained on NS (LSns, NSns and HSns). Echocardiogram was repeated at 30 weeks of age. Mean blood pressure (MBP), histology and left ventricular protein and gene expression of the renin-angiotensin system components were analyzed at 36 weeks of age. LS or HS diet during pregnancy was not associated with cardiac abnormalities in adult male offspring until the 36th week of age, when maintained on a NS diet. HShs offspring group presented a blood pressure and angiotensin II independent concentric left ventricular hypertrophy, with no fibrosis. Surprisingly, MBP was lower (p<0.05) in LShs offspring compared to HShs, NShs and LSns. Although we did not verify signs of left ventricular hypertrophy in offsprings from dams fed a LS diet, cardiac output was lower in LShs compared to HShs (p<0.05) and NShs (p=0.06) and average number of nuclei per cardiomyocyte was higher (p<0.05) in LShs compared to LSns offspring groups.

Cloreto de sódio

Gestação

Hipertrofia ventricular esquerda

Programação fetal

Ratos Wistar

Sistema renina-angiotensina

Fetal programming

Left ventricular hypertrophy

Pregnancy

Renin-angiotensin system

Sodium chloride

Wistar rats

Cardiovascular Fetal Programming in Quail (Colinus virginianus), An Avian Comparative Model

Flores Santin, Josele R.

12 1900

The consequences of early embryonic insults and how they affect subsequent life reflects the emerging concept of "fetal programming". The aim of this project is to study the effects of embryonic insults as they subsequently manifest themselves in adults, with emphasis on the heart and vasculature. My experiments establish that fetal programming operates on the bobwhite quail inducing similar changes as those observed in mammalians and other birds. The quail's fast development provides reliable data in a short period of time than other avian models (e.g. domestic chicken). Data on quail showed a correlation between egg mass and hatchling mass; where small eggs produce small hatchlings but a high mortality made it impractical as a stressor for this study. Hypoxia was used as a stressor during embryonic incubation, where it induced a low hatching weight in quail that was not observable in adult birds. Morphological measurements demonstrated an increased ventricular collagen content and reduced ventricular lumen in birds in adults incubated in hypoxia consistent with hypertension. The hematological analyzes showed few differences indicating organ remodeling instead of hematopoietic compensation. The assessment of vascular reactivity pointed out an impaired endothelium dependent relaxation commonly associated to hypertension in birds and mammals. Fetal programming could be a widespread response to an adverse prenatal environment in endotherms and the resulting data from this work contributes to our understanding of fetal programming in vertebrates and its long term consequences.

fetal programming

avian models

bobwhite quail

embryonic insults

cardiovascular reactivity

Fetus -- Development.

Fetal distress.

Fetal anoxia.

Hypertension -- Etiology.

Northern bobwhite -- Embryology.

Programação fetal por restrição proteica avaliação estrutural da próstata ventral de ratos wistar /

Freitas, Selma de Bastos Zambelli

January 2020

Orientador: Patricia Fernanda Felipe Pinheiro / Resumo: A programação fetal (PF) é o resultado permanente do organismo na presença de estímulos ocorridos durante os períodos críticos de desenvolvimento. Vários fatores ambientais podem levar à PF. Entre eles, podemos citar a restrição alimentar materna ou a deficiência específica de nutrientes. De acordo com a janela de programação fetal masculinizante (MPW), os andrógenos agem para assegurar o desenvolvimento normal dos órgãos reprodutores do macho, assim, foram estudados os efeitos da restrição proteica materna durante a gestação e lactação sobre o desenvolvimento da próstata ventral de ratos Wistar. Para isto, dois grupos de ratas gestantes foram alimentadas com dietas isocalóricas, sendo um grupo normoproteico (NP) e o outro grupo hipoproteico (RP). Os grupos NP e RP tiveram livre acesso à dieta durante os períodos de gestação e lactação. Após o desmame, metade da prole de machos foi eutanasiada. A outra metade da prole de machos recebeu dieta padrão de animais de laboratório até os 120 dias de idade. A próstata ventral foi estudada por imuno-histoquímica para a avaliação da localização do antígeno de proliferação celular (PCNA), da proteína p63, dos receptores de andrógeno (AR), de estrógeno alfa (ER-α), de grelina (GHSR-1a), de leptina (Ob -R). Os pesos corpóreo, da próstata ventral, dos testículos e do tecido adiposo e os níveis de testosterona e estradiol foram obtidos. A PF determinou atraso no crescimento somático dos animais do grupo RP e diminuição do estradiol plasmáti... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Fetal programming (FP) is the permanent result of the organism in the presence of stimuli during the periods of development. Several environmental factors can lead to FP. Among them, we can mention the maternal food restriction or deficiency of specific nutrients. According to the masculinization programming window (MPW) in which androgens act to ensure normal development of the male reproductive organs, we studied the effects of maternal protein restriction during pregnancy and lactation period on the development of the Wistar rat ventral prostate. Dams of the group (NP) were fed diet containing 17% protein; Dams of the group (RP) were fed diet containing 8% protein. The NP and RP groups had free access to diet during pregnancy and lactation period. After weaning, half of the male pups was killed. The other half of male pups received a standard laboratory diet until 120 days old. The ventral prostate was studied immunohistochemically to evaluate the expression of cell proliferation antigen (PCNA), p63 protein, androgen (AR), alpha estrogen (ER-α), ghrelin (GHSR-1a), leptin (Ob -R) receptors. The body, ventral prostate, testes and adipose tissue weights, testosterone and estradiol levels were determined. FP determined a delay somatic growth of the RP group and decrease of the plasmatic estradiol of the adult animals of the RP group. At 21 days of age, the RP group presented less intense immunostaining for ER-α, GHSR-1a, and Ob-R when compared to the NP group. At 120 days, the... (Complete abstract click electronic access below) / Doutor

Desenvolvimento fetal.

Receptor de andrógeno (AR)

Receptor de leptina (Ob-R)

Receptor de grelina (GHS-R 1a)

Receptor de estrógeno

Próstata.

Proliferação celular (PCNA)

Fetal programming

Androgen receptor (AR)

Prostate

Le transcriptome et le méthylome du foie des rats dénutris en période périnatale identifient les gènes principaux impliqués dans les pathologies métaboliques / The liver transcriptome and methylome of rat perinatally malnourished identify keys genes involved in metabolic diseases

Chen, Gaili

28 November 2014

Une des caractéristiques les plus connues de la programmation métabolique est qu’un événement commun physiopathologique à l'âge adulte obtenu indépendamment du stress nutritionnel au début de la vie. Cela a conduit à penser que les altérations métaboliques dûes au stress nutritionnel précoce pouvaient résulter de la programmation seulement d’un petit nombre de gènes qui agissent comme gardiens d'un réseau de gènes ou d'une voie de signalisation. Ici nous avons l’intention de tester cette hypothèse par l'analyse combinée du transcriptome et méthylome avec des échantillons de foie des rats nés de mères nourries avec une alimentation restreinte en protéines (MPR) ou carencée en donneur de méthyles (MDD) pendant la gestation et la lactation et comparer entre les 2 modèls. Au moment du sevrage, la progéniture MDD a été sacrifiée, tandis que la progéniture du groupe MPR a reçu une nourriture standard jusqu'à l'âge de 6 mois. Les rats à jours 21 nés de mères nourries avec un régime MDD ont 3.269 gènes surexprimé (P <0,0009) et 2.841 gènes sous-exprimés (P <0,0004) par rapport aux témoins. Les modifications de méthylation de l'ADN ont été trouvées dans les régions promotrices de 1.032 gènes. Les analyses fonctionnelles ont révélé que ces gènes sont principalement impliqués dans le métabolisme des lipides et du glucose, du système nerveux, la coagulation, le stress du réticulum endoplasmique et la fonction mitochondriale. Les master genes présentant des changements à la fois dans l'expression et la méthylation d'ADN sont limités à 266 gènes et ils sont principalement impliqués dans le système rénine-angiotensine, le métabolisme de la mitochondrie et de l'homéostasie phospholipide. La plupart de ces master genes participent à la Non Alcoholic Fatty Liver Disease (NAFLD). La restriction protéique maternelle (MPR) a entraîné une augmentation de la masse grasse abnominale, de l'hypertriglycéridémie, de l'hypercholestérolémie et un taux élevé d’acides gras par rapport aux témoins. 3.020 gènes sont surexprimés (P<0,0003) et 3.601 sous-exprimés (P<0,002) au niveau du transcriptome et 3.968 gènes modifiés au niveau du méthylome par rapport aux témoins. L'analyse fonctionnelle a indiqué que les gènes surexprimés sont principalement impliqués dans les voies métaboliques et les gènes sous-exprimés et différemment méthylés sont principalement impliqués dans des processus du développement. 998 master genes ont été trouvés, et léanalyse fonctionnelle de ces gènes a indiqué un effet significatif sur le développement des tissus, la régulation de la transcription et le métabolisme, et beaucoup d'entre eux sont associés à des maladies chroniques comme l'hypertension, l'obésité centrale et le diabète. L'expression des gènes et la méthylation de l'ADN du génome obtenus en utilisant ces modèles ont été comparés aux données de méthylome et de transcriptome précédemment obtenus à partir de foie des rats restreints en protéines et sacrifiés à la naissance. Cette analyse a révélé un ensemble commun de 46 gènes qui sont sur-exprimés et 42 gènes sous-exprimés dans les trois modèles de programmation métabolique par rapport aux animaux témoins. La plupart des gènes surexprimés sont impliqués dans la régulation de la fonction mitochondriale alors que les gènes sous-exprimés sont principalement impliquées dans la régulation de la prolifération cellulaire et l'expression des gènes. Nous avons identifié également un ensemble de 122 gènes dont les niveaux de méthylation ont été modifiés à la fois par une carence en donneurs de méthyle et une restriction protéique. Ces observations soutiennent l’hypothèse qu’un petit nombre de gènes essentiels sont à la base de la programmation de troubles métaboliques, indépendamment du stress nutritionnel / One of the most striking features of metabolic programming is that a common physiopathological output at adulthood is obtained irrespective to the nutritional insult during early life. This has suggested that the metabolic alterations due to early nutritional stress might result from the programming of only a small number of genes which act as gatekeepers of a fundamental gene network or signalling pathway. Here we aimed to test this hypothesis through the combined analysis of the transcriptome and methylome in rat liver samples derived from animals born to dams fed either a protein-restricted diet (MPR) or a methyl donor deficient (MDD) diet through gestation and lactation. At weaning, the offspring born to MDD dams were sacrificed whereas the pups from the MPR group were fed standard chow until the age of 6 months. 21-day-old rats born to mothers fed a MDD diet during gestation and lactation have 3,269 over-expressed (P<0.0009) and 2,841 under-expressed (P<0.0004) genes compared to controls. Modifications of DNA methylation were found in the promoter regions of 1,032 genes. Functional analyses revealed that these genes are mainly involved in glucose and lipid metabolism, nervous system, coagulation, endoplasmic reticulum stress and mitochondrial function. Master genes exhibiting changes in both gene expression and DNA methylation are limited to 266 genes and are mainly involved in the renin-angiotensin system, mitochondrion metabolism and phospholipid homeostasis. Most of these master genes participate in Non Alcoholic Fatty Liver Disease (NAFLD). Maternal protein restriction (MPR) resulted in increased fat mass, hypertriglyceridemia, hypercholesterolemia and high fatty acids compared to control. 3,020 genes were up-regulated (p < 0.0003) and 3,601 (p ? 0.002) down-regulated by MPR compared to controls. Modifications of DNA methylation was found in 3,968 genes. The functional analysis indicated that the overexpressed genes were mainly involved in metabolic pathways and the under-expressed and differentially methylated genes were mainly involved in physiological process. 998 master genes were found, functional analysis of these genes indicated a significant effect on tissue development, regulation of transcription and metabolism, and many of them are associated with chronic diseases such as hypertension, central obesity and diabetes. The genome-wide expression and DNA metylation results obtained using these models, were compared to previous methylome and transcriptome data obtained using liver from MPR pups sacrificed at birth. This analysis revealed a common set of 46 genes that were up regulated and 42 genes down regulated in the three models of metabolic programming compared to control animals. Most of the up regulated genes are involved in the regulation of mitochondrial function whereas the down-regulated genes are mainly involved in the regulation of cell proliferation and gene expression. We identified also a set of 122 genes whose methylation levels were changed both by methyl donor deficiency and protein-restriction. These observations sustain the hypothesis that a small set of core genes underlies the programming of metabolic disorders irrespective of the nutritional insult

Programmation métabolique

Programmation fœtale

Épigénétique

Méthylation de l'ADN

Restriction protéique maternelle

Carence en donneurs de méthyle

Méthylome

Metabolic programming

Fetal programming

Epigenetics

DNA methylation

Maternal protein restriction

Methyl donor deficiency

Methylome

572.8

576.53