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Efeitos da reposição terapêutica central de melatonina em animais pinealectomizados - implicações no comportamento alimentar e peso corporal. / Effects of therapeutic central replacement of melatonin in pinealectomized animals - implications on feeding behavior and body weight.Ferreira, Rosana Fátima Dantas 12 February 2015 (has links)
A melatonina é um hormônio que possui ritmos circulatórios robustos e previsíveis. Em animais pinealectomizados a concentração plasmática de melatonina é abolida e acompanha alterações fisiológicas como resistência à insulina e desequilíbrio entre requerimento e mobilização energética do tecido adiposo. Este estudo objetivou avaliar os efeitos da suplementação de melatonina central, através de injeção intracerebroventricular (ICV). Os resultados obtidos indicam que a pinealectomia, provoca um aumento do consumo alimentar e um considerável aumento de peso. Mostrou-se, ainda, que a reposição ICV de melatonina é capaz de provocar a diminuição do consumo alimentar, assim como uma diminuição expressiva do peso corporal. Observou-se, também, que a administração de melatonina nos animais controles regularizam o peso corpóreo, impedindo o aumento de peso próprio do avançar da idade e que a melatonina foi um agente importante na redução de gordura corporal. / Melatonin is a hormone with robust and predictable rhythms being a strong synchronizer for the expression of several physiological processes. But in pinealectomized rats plasma concentration of melatonin is abolished, leading to physiological changes such as insulin resistance and imbalance between energy requirement and mobilization from adipose tissue. The aim of the study was to evaluate the effects of intracerebroventricular supplementation of melatonin. We studied food intake, weight gain and peripheral insulin sensitivity. The results obtained indicate that the pinealectomy caused an increase in food consumption and a considerable weight gain. Furthermore, icv melatonin replacement in these animals counteracted both effects. It was observed also that melatonin in control animals regulates body weight, preventing weight gain characteristic of aging. Finally, it was also observed that melatonin-induced decrease in body weight is due to a reduction of fat adipose tissues.
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Efeitos da reposição terapêutica central de melatonina em animais pinealectomizados - implicações no comportamento alimentar e peso corporal. / Effects of therapeutic central replacement of melatonin in pinealectomized animals - implications on feeding behavior and body weight.Rosana Fátima Dantas Ferreira 12 February 2015 (has links)
A melatonina é um hormônio que possui ritmos circulatórios robustos e previsíveis. Em animais pinealectomizados a concentração plasmática de melatonina é abolida e acompanha alterações fisiológicas como resistência à insulina e desequilíbrio entre requerimento e mobilização energética do tecido adiposo. Este estudo objetivou avaliar os efeitos da suplementação de melatonina central, através de injeção intracerebroventricular (ICV). Os resultados obtidos indicam que a pinealectomia, provoca um aumento do consumo alimentar e um considerável aumento de peso. Mostrou-se, ainda, que a reposição ICV de melatonina é capaz de provocar a diminuição do consumo alimentar, assim como uma diminuição expressiva do peso corporal. Observou-se, também, que a administração de melatonina nos animais controles regularizam o peso corpóreo, impedindo o aumento de peso próprio do avançar da idade e que a melatonina foi um agente importante na redução de gordura corporal. / Melatonin is a hormone with robust and predictable rhythms being a strong synchronizer for the expression of several physiological processes. But in pinealectomized rats plasma concentration of melatonin is abolished, leading to physiological changes such as insulin resistance and imbalance between energy requirement and mobilization from adipose tissue. The aim of the study was to evaluate the effects of intracerebroventricular supplementation of melatonin. We studied food intake, weight gain and peripheral insulin sensitivity. The results obtained indicate that the pinealectomy caused an increase in food consumption and a considerable weight gain. Furthermore, icv melatonin replacement in these animals counteracted both effects. It was observed also that melatonin in control animals regulates body weight, preventing weight gain characteristic of aging. Finally, it was also observed that melatonin-induced decrease in body weight is due to a reduction of fat adipose tissues.
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Alterações motoras, comportamentais e histopatológicas após injeção intracerebroventricular de liquor de pacientes com esclerose lateral amiotrófica em ratos / Motor, behavioral and histopathological changes after intracerebroventricular cerebrospinal fluid injection of patients with amyotrophic lateral sclerosis in ratsGois, Auderlan Mendonça de 26 February 2016 (has links)
Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / Amyotrophic Lateral Sclerosis (ALS) is a progressive neurodegenerative disease that
affects the somatic motor system through the degeneration of upper and lower
motors neurons. Evidence suggests that the cerebrospinal fluid (CSF), which is in
direct contact with the nervous system, has soluble substance that could cause
injuries in motor neurons. Animal models that express mutant ALS associated genes
have been created to study the various etiopathological mechanisms which manifest
themselves similarly to that occur in ALS patients. However, these models best
represent the etiology of the disease in familiar cases and there is not yet an animal
model that represents the characteristics of the disease in sporadic form, despite the
similarity between familiar and sporadic cases. Thus, the aim of this study was to
evaluate the motor and histological changes after intracerebroventricular injection
(i.c.v.) of CSF from ALS sporadic patients in rats. 43 seven-month-old Wistar rats
were used, coming from the sectoral animal facility of the Department of Physiology
at the Federal University of Sergipe. The study was divided into two experiments: (I)
with a single administration i.c.v. of the CSF and (II) with repeated administration
i.c.v. of the CSF. In the experiment I, the animals were divided into 3 groups: control
(CTR, artificial CSF solution), non-ALS (N-ALS, CSF of patients without neurological
disease) and ALS (ALS, LCR of patients with sporadic ALS) who received a single
injection i.c.v. (7.5μL) and one week after were subjected to motor tests: strength
test, catalepsy test, open field test and walking test once a week for 30 days. In the
Experiment II, animals were divided into 3 groups: control (CTR) Non-ALS (N-ALS)
and ALS and they received daily injection for 6 days, i.c.v. (5.0μL). Throughout the
treatment the animals underwent the motor tests already mentioned. After the tests,
in both experiments, rats were anesthetized, perfused, their spinal cords were
removed and subjected to histological analysis by hematoxylin-eosin for general
morphological observation. In the first experiment ,in ALS group, motor alteration was
observed in the strength test, open field and in the walking test, accompanied by a
reduction of motor neurons and glial cells in the thoracic and lumbar regions of the
spinal cord. In the second experiment, Also in the ALS group, it was observed driving
change in catalepsy, open field and in the walking test, accompanied by an increase
of glial cells in the lumbar region of the spinal cord. Data presented in this study show
that the CSF management of ALS patients can cause pathogenic mechanisms
similar to those seen in humans and other animal models of ALS. / A Esclerose Lateral Amiotrófica (ELA) é uma doença neurodegenerativa progressiva,
que afeta o sistema motor somático através da degeneração dos neurônios motores
superiores e inferiores. Evidências apontam que o líquido cefalorraquidiano (LCR),
que está em íntimo contato com o sistema nervoso, apresenta substâncias solúveis
que podem provocar lesões em neurônios motores. Modelos animais que expressam
genes mutantes associados à ELA foram desenvolvidos, para o estudo dos mais
diversos mecanismos etiopatológicos que se manifestam de forma similar aos que
ocorrem em pacientes com a doença. Entretanto, esses modelos representam
melhor a etiologia da doença em casos familiares e, apesar da semelhança entre
casos familiares e esporádicos, ainda não se tem um modelo animal que represente
características da doença nesta última. Diante disso, o objetivo do presente trabalho
foi avaliar as alterações motoras e histológicas após injeção intracerebroventricular
(i.c.v.) de LCR de pacientes com ELA esporádica em ratos Wistar. Foram ultilizados
43 ratos Wistar, com idade aproximada de sete meses, provenientes do Biotério
Setorial do Departamento de Fisiologia da Universidade Federal de Sergipe. O
trabalho foi dividido em 2 experimentos: (I) com uma única administração i.c.v. de
LCR e (II) com administrações repetidas i.c.v. de LCR. No experimento I os animais
foram divididos em 3 grupos, controle (CTR, solução de LCR artificial), não-ELA (NELA,
LCR de pacientes sem doenças neurológicas) e ELA (ELA, LCR de paciente
com ELA esporádica) que receberam uma única injeção i.c.v. de 7,5 μL e após uma
semana foram submetidos aos testes motores: teste de força, catalepsia, campo
aberto e teste de marcha uma vez por semana durante 30 dias. No experimento II,
os animais foram divididos em 3 grupos, controle (CTR), Não-ELA (N-ELA) e ELA
que receberam uma injeção diária, durante 6 dias, i.c.v. de 5 μL. Ao longo do
tratamento, os animais foram submetidos aos testes motores acima mencionados.
Após os testes, em ambos experimentos, os ratos foram anestesiados, perfundidos,
suas medulas removidas e submetidas à análise histológica pela coloração de
hematoxilina-eosina para observação morfológica geral. No experimento I, no grupo
ELA, foi observado alteração motora no teste de força, campo aberto e no teste de
marcha, acompanhado por uma redução de neurônios motores e células gliais na
região torácica e lombar da medula espinal. No experimento II, também no grupo
ELA, foi observado alteração motora na catalepsia, campo aberto e no teste de
marcha, acompanhado de um aumento de células gliais na região lombar da medula
espinal. Os dados apresentados neste estudo mostram que a administração de LCR
de pacientes com ELA pode provocar mecanismos patogênicos semelhantes aos
observados em humanos e outros modelos animais de ELA.
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The Duodenal Mucosal Bicarbonate Secretion : Role of Melatonin in Neurohumoral Control and Cellular SignalingSjöblom, Markus January 2003 (has links)
<p>The duodenal lumen is exposed to aggressive factors with a high potential to cause damage to the mucosa. Bicarbonate secretion by the duodenal mucosa is accepted as the primary important defense mechanism against the hydrochloric acid intermittently expelled from the stomach.</p><p>The present thesis concerns the influence of the central nervous system and the effects of the hormone melatonin on bicarbonate secretion in anesthetized rats in vivo. Effects of melatonin on intracellular calcium signaling by duodenal enterocyte in vitro were examined in tissues of both human and rat origin. The main findings were as follows:</p><p>Melatonin is a potent stimulant of duodenal mucosal bicarbonate secretion and also seems to be involved in the acid-induced stimulation of the secretion. Stimulation elicited in the central nervous system by the α1-adrenoceptor agonist phenylephrine induced release of melatonin from the intestinal mucosa and a four-fold increase in alkaline secretion. The melatonin antagonist luzindole abolished the duodenal secretory response to administered melatonin and to central nervous phenylephrine but did not influence the release of intestinal melatonin. Central nervous stimulation was also abolished by synchronous ligation of the vagal trunks and the sympathetic chains at the sub-laryngeal level. </p><p>Melatonin induced release of calcium from intracellular stores and also influx of extracellular calcium in isolated duodenal enterocytes. Enterocytes in clusters functioned as a syncytium.</p><p>Overnight fasting rapidly and profoundly down-regulated the responses to the duodenal secretagogues orexin-A and bethanechol but not those to melatonin or vasoactive intestinal polypeptide.</p><p>In conclusion, the results strongly suggest that intestinal melatonin plays an important role in central nervous elicited stimulation of duodenal mucosal bicarbonate secretion. Sensitivity of this alkaline secretion to some peripheral stimulators markedly depends on the feeding status.</p>
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The Duodenal Mucosal Bicarbonate Secretion : Role of Melatonin in Neurohumoral Control and Cellular SignalingSjöblom, Markus January 2003 (has links)
The duodenal lumen is exposed to aggressive factors with a high potential to cause damage to the mucosa. Bicarbonate secretion by the duodenal mucosa is accepted as the primary important defense mechanism against the hydrochloric acid intermittently expelled from the stomach. The present thesis concerns the influence of the central nervous system and the effects of the hormone melatonin on bicarbonate secretion in anesthetized rats in vivo. Effects of melatonin on intracellular calcium signaling by duodenal enterocyte in vitro were examined in tissues of both human and rat origin. The main findings were as follows: Melatonin is a potent stimulant of duodenal mucosal bicarbonate secretion and also seems to be involved in the acid-induced stimulation of the secretion. Stimulation elicited in the central nervous system by the α1-adrenoceptor agonist phenylephrine induced release of melatonin from the intestinal mucosa and a four-fold increase in alkaline secretion. The melatonin antagonist luzindole abolished the duodenal secretory response to administered melatonin and to central nervous phenylephrine but did not influence the release of intestinal melatonin. Central nervous stimulation was also abolished by synchronous ligation of the vagal trunks and the sympathetic chains at the sub-laryngeal level. Melatonin induced release of calcium from intracellular stores and also influx of extracellular calcium in isolated duodenal enterocytes. Enterocytes in clusters functioned as a syncytium. Overnight fasting rapidly and profoundly down-regulated the responses to the duodenal secretagogues orexin-A and bethanechol but not those to melatonin or vasoactive intestinal polypeptide. In conclusion, the results strongly suggest that intestinal melatonin plays an important role in central nervous elicited stimulation of duodenal mucosal bicarbonate secretion. Sensitivity of this alkaline secretion to some peripheral stimulators markedly depends on the feeding status.
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Nutritional regulation of central fat mass and obesity-associated (FTO) expression, and its association with the central melanocortin signaling in the regulation of energy homeostasisPoritsanos, Nicole Joanna 22 November 2010 (has links)
The central nervous system (CNS) melanocortin signaling pathway plays a critical role in the regulation of metabolism. However, the regulatory effects of CNS melanocortin signaling on hepatic lipid metabolism and fatty liver disease have not been well established. Although the activity of the CNS melanocortin system is regulated by metabolic signals, the mechanism for this regulation is not fully understood. Variants of the FTO (fat mass and obesity-associated) gene are associated with obesity and FTO is expressed in the hypothalamic neurons including proopiomelanocortin (POMC) neurons. Therefore, it is hypothesized that hypothalamic FTO plays a role in the regulation of metabolism by mediating the effect of metabolic signals on hypothalamic melanocortinergic neurons, and that impairments in this regulation may cause metabolic impairments including obesity and fatty liver disease.
Intracerebroventricular (i.c.v.) treatment with SHU9119, a melanocortin antagonist, increased hepatic lipid accumulation and the expression of genes encoding lipogenic enzymes in lean mice. Conversely, i.c.v. treatment with MTII, a melanocortin agonist, reduced the expression of hepatic lipogenic genes in association with reduction in body weight in ob/ob mice, a mouse model of fatty liver disease.
Immunohistochemical analysis demonstrated that Fto is co-expressed in both POMC and agouti-related protein (AgRP) neurons in the mouse hypothalamus. Fto mRNA and protein expression was reduced by fasting and increased by glucose treatment in nutritionally important hypothalamic nuclei. Fasting-induced reduction in hypothalamic Fto expression was observed in both lean wild-type and obese ob/ob mice, while the stimulatory effect of glucose on hypothalamic Fto expression was absent in ob/ob mice.
These findings support the hypothesis that central melanocortin signaling regulates hepatic lipid metabolism in part by regulating de novo lipogenesis. Impairments in the central melanocortin signaling lead to the development of hepatic steatosis, while enhanced melanocortin signaling may be beneficial in reversing abnormal hepatic lipid metabolism in fatty liver disease (Poritsanos et al., 2008). These findings also support the hypothesis that Fto is expressed in the hypothalamic melanocortinergic neurons and is regulated by metabolic signals involving changes in CNS glucose availability and/or glucose action. Impairments in this regulation may cause metabolic impairments including obesity and fatty liver disease.
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Nutritional regulation of central fat mass and obesity-associated (FTO) expression, and its association with the central melanocortin signaling in the regulation of energy homeostasisPoritsanos, Nicole Joanna 22 November 2010 (has links)
The central nervous system (CNS) melanocortin signaling pathway plays a critical role in the regulation of metabolism. However, the regulatory effects of CNS melanocortin signaling on hepatic lipid metabolism and fatty liver disease have not been well established. Although the activity of the CNS melanocortin system is regulated by metabolic signals, the mechanism for this regulation is not fully understood. Variants of the FTO (fat mass and obesity-associated) gene are associated with obesity and FTO is expressed in the hypothalamic neurons including proopiomelanocortin (POMC) neurons. Therefore, it is hypothesized that hypothalamic FTO plays a role in the regulation of metabolism by mediating the effect of metabolic signals on hypothalamic melanocortinergic neurons, and that impairments in this regulation may cause metabolic impairments including obesity and fatty liver disease.
Intracerebroventricular (i.c.v.) treatment with SHU9119, a melanocortin antagonist, increased hepatic lipid accumulation and the expression of genes encoding lipogenic enzymes in lean mice. Conversely, i.c.v. treatment with MTII, a melanocortin agonist, reduced the expression of hepatic lipogenic genes in association with reduction in body weight in ob/ob mice, a mouse model of fatty liver disease.
Immunohistochemical analysis demonstrated that Fto is co-expressed in both POMC and agouti-related protein (AgRP) neurons in the mouse hypothalamus. Fto mRNA and protein expression was reduced by fasting and increased by glucose treatment in nutritionally important hypothalamic nuclei. Fasting-induced reduction in hypothalamic Fto expression was observed in both lean wild-type and obese ob/ob mice, while the stimulatory effect of glucose on hypothalamic Fto expression was absent in ob/ob mice.
These findings support the hypothesis that central melanocortin signaling regulates hepatic lipid metabolism in part by regulating de novo lipogenesis. Impairments in the central melanocortin signaling lead to the development of hepatic steatosis, while enhanced melanocortin signaling may be beneficial in reversing abnormal hepatic lipid metabolism in fatty liver disease (Poritsanos et al., 2008). These findings also support the hypothesis that Fto is expressed in the hypothalamic melanocortinergic neurons and is regulated by metabolic signals involving changes in CNS glucose availability and/or glucose action. Impairments in this regulation may cause metabolic impairments including obesity and fatty liver disease.
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Effects of Orexins, Guanylins and Feeding on Duodenal Bicarbonate Secretion and Enterocyte Intracellular SignalingBengtsson, Magnus Wilhelm January 2008 (has links)
<p>The duodenal epithelium secretes bicarbonate ions and this is regarded as the primary defence mechanism against the acid discharged from the stomach. For an efficient protection, the duodenum must also function as a sensory organ identifying luminal factors. Enteroendocrine cells are well-established intestinal “taste” cells that express signaling peptides such as orexins and guanylins. Luminal factors affect the release of these peptides, which may modulate the activity of nearby epithelial and neural cells.</p><p>The present thesis considers the effects of orexins and guanylins on duodenal bicarbonate secretion. The duodenal secretory response to the peptides was examined in anaesthetised rats <i>in situ</i> and the effects of orexin-A on intracellular calcium signaling by human as well as rat duodenal enterocytes were studied <i>in vitro</i>.</p><p>Orexin-A, guanylin and uroguanylin were all stimulants of bicarbonate secretion. The stimulatory effect of orexin-A was inhibited by the OX<sub>1</sub>-receptor selective antagonist SB-334867. The muscarinic antagonist atropine on the other hand, did not affect the orexin-A-induced secretion, excluding involvement of muscarinic receptors. Orexin-A induced calcium signaling in isolated duodenocytes suggesting a direct effect at these cells. Interestingly, orexin-induced secretion and calcium signaling as well as mucosal orexin-receptor mRNA and OX<sub>1</sub>-receptor protein levels were all substantially downregulated in overnight fasted rats compared with animals with continuous access to food. Further, secretion induced by Orexin-A was shown to be dependent on an extended period of glucose priming.</p><p>The uroguanylin-induced bicarbonate secretion was reduced by atropine suggesting involvement of muscarinic receptors. The melatonin receptor antagonist luzindole attenuated the secretory response to intra-arterially administered guanylins but had no effect on secretion when the guanylins were given luminally. </p><p>In conclusion, the results suggest that orexin-A as well as guanylins may participate in the regulation of duodenal bicarbonate secretion. Further, the duodenal orexin system is dependent on the feeding status of the animals.</p>
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Effects of Orexins, Guanylins and Feeding on Duodenal Bicarbonate Secretion and Enterocyte Intracellular SignalingBengtsson, Magnus Wilhelm January 2008 (has links)
The duodenal epithelium secretes bicarbonate ions and this is regarded as the primary defence mechanism against the acid discharged from the stomach. For an efficient protection, the duodenum must also function as a sensory organ identifying luminal factors. Enteroendocrine cells are well-established intestinal “taste” cells that express signaling peptides such as orexins and guanylins. Luminal factors affect the release of these peptides, which may modulate the activity of nearby epithelial and neural cells. The present thesis considers the effects of orexins and guanylins on duodenal bicarbonate secretion. The duodenal secretory response to the peptides was examined in anaesthetised rats in situ and the effects of orexin-A on intracellular calcium signaling by human as well as rat duodenal enterocytes were studied in vitro. Orexin-A, guanylin and uroguanylin were all stimulants of bicarbonate secretion. The stimulatory effect of orexin-A was inhibited by the OX1-receptor selective antagonist SB-334867. The muscarinic antagonist atropine on the other hand, did not affect the orexin-A-induced secretion, excluding involvement of muscarinic receptors. Orexin-A induced calcium signaling in isolated duodenocytes suggesting a direct effect at these cells. Interestingly, orexin-induced secretion and calcium signaling as well as mucosal orexin-receptor mRNA and OX1-receptor protein levels were all substantially downregulated in overnight fasted rats compared with animals with continuous access to food. Further, secretion induced by Orexin-A was shown to be dependent on an extended period of glucose priming. The uroguanylin-induced bicarbonate secretion was reduced by atropine suggesting involvement of muscarinic receptors. The melatonin receptor antagonist luzindole attenuated the secretory response to intra-arterially administered guanylins but had no effect on secretion when the guanylins were given luminally. In conclusion, the results suggest that orexin-A as well as guanylins may participate in the regulation of duodenal bicarbonate secretion. Further, the duodenal orexin system is dependent on the feeding status of the animals.
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