Teses / dissertações sobre o tema "Insulin metabolism"
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Vidal, Alabró Anna. "Estudi de l’activació de la glucocinasa (GKA456V) en fetge perivenós". Doctoral thesis, Universitat de Barcelona, 2011. http://hdl.handle.net/10803/32022.
Texto completo da fonteSynthetic glucokinase activators have been used in the context of type 2 diabetes therapy, mainly for their insulin secretagogue activity. However, the impact of these drugs on liver GK has not been studied in vivo. Since GK activators and activating GK mutations confer identical kinetic properties to GK, we hypothesize that hepatic overexpression of a mutated form of GK, GKA456V, described in a patient with Persistent Hyperinsulinemic Hypoglycemia of Infancy (PHHI), shall mimic the liver-specific effects of GK-activating drugs. GKA456V was overexpressed in the liver of streptozotocin diabetic mice and also in healthy mice. Metabolite profiling in serum and liver extracts, together with key components of glucose and lipid homeostasis, were analyzed and compared to GK wild-type transfected animals. Cell compartmentalization of mutant and wild-type GK was also examined in vivo. In the type 1 diabetic mice, GKA456V overexpression markedly reduced blood glucose in the absence of dislipidemia, in contrast to wild-type GK-overexpressing mice. Enhanced glucose utilization did not correlate with glycogen synthesis or lactate production. PEPCK mRNA was not affected, whereas the mRNA for the catalytic subunit of glucose-6-phosphatase was upregulated ~4-fold in the liver of GKA456V treated animals. Moreover, GKA456V was not translocated to the nucleus after a short fast, confirming that this activating mutation disrupted GKRP regulation. In healthy mice, the overexpression of hepatic GK resulted in insulin resistance. Otherwise, GKA456V overepxressing animals were not insulin resistant. They showed increased mRNA and protein content of the catalytic subunit of glucose-6-phosphatase in the liver, and an idnuction of catabolism in their adipose tissue. Our results validate liver specific GK activation as a strategy for diabetes therapy and provide new insights into the complex GK regulatory network.
Collison, Mary Williamson. "Insulin signalling in insulin resistance and cardiovascular disease syndromes". Thesis, University of Glasgow, 2001. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.366184.
Texto completo da fonteKershner, David. "Oral Glucose Insulin Secretion Test for Identifying Patients with Insulin Resistance". ScholarWorks, 2018. https://scholarworks.waldenu.edu/dissertations/5634.
Texto completo da fonteMashhedi, Haider. "Implicating insulin in neoplastic growth and metabolism". Thesis, McGill University, 2011. http://digitool.Library.McGill.CA:80/R/?func=dbin-jump-full&object_id=104681.
Texto completo da fonteCompte tenu de l'accumulation de preuves liant l'obésité à un nombre accru de cancers, il y a un grand intérêt à définir les mécanismes par lesquels l'obésité influe sur la croissance néoplasique. Des niveaux d'insuline élevés sont couramment associés à l'obésité ou au «syndrome métabolique», ce qui fait que le récepteur de l'insuline est considéré comme une cible moléculaire potentiellement importante pour le traitement de certains cancers. Pour étudier les effets de l'atténuation de la signalisation de l'insuline sur la croissance du modèle expérimental du cancer du sein chez la souris, la lignée cellulaire insulino-sensible 4T1 in vivo, nous avons comparé les effets d'une déficience à l'insuline induite par l'alloxan à celle de BMS-536924, un inhibiteur des kinases tyrosine des récepteurs de l'insuline et d'IGF-I. Les deux interventions ont montré une activité anti-néoplasique, mais seulement l'alloxan a présenté une toxicité métabolique. L'inhibition des récepteurs d'insuline n'a occasionné qu'une faible hyperglycémie et le traitement avec BMS-536924 a été bien toléré. Nous avons attribué ce phénomène à des facteurs pharmacocinétiques en mesurant l'accumulation de drogue dans les tissus et pour déterminer si le BMS-536924 abolit l'absorption insulino-dépendante du glucose, nous avons mesuré la quantité de glucose utilisé dans le muscle. Nos données indiquent que la captation insulino-dépendante du glucose par le muscle est restée intacte. Ainsi, la distribution tissu-spécifique du BMS-536924 peut être responsable de l'activité anti-néoplasique sans toxicité métabolique grave, ce qui indique que le ciblage pharmacologique du récepteur de l'insuline dans la maladie néoplasique peut être efficace.Les études épidémiologiques ont montré que les patients diabétiques de type II prenant le médicament metformine (un biguanide) ont un risque réduit de développer un cancer ou d'un taux de mortalité due au cancer plus faible par rapport aux patients diabétiques de type II suivant d'autres thérapies. Nous avons déjà montré que la metformine agit comme un inhibiteur de la croissance des cellules tumorales in vitro en phosphorylant l'AMPK d'une manière dépendante de la dose. Outre l'activation de l'AMPK, qui est observée dans les cellules tumorales in vitro et in vivo, la metformine provoque aussi une diminution des taux d'insuline. Ceci est un effet secondaire de la réduction du taux de glycémie dans un contexte de diabète de type II. La tomographie par émission de positons (TEP ou PET) est une technique d'imagerie qui mesure le taux d'utilisation du glucose par les cellules cancéreuses à l'aide de l'analogue du glucose radiomarqué 18F-2-Fluoro-2-Désoxy-D-Glucose (FDG). Nous étions intéressés par les effets de la metformine sur la captation du glucose par les tumeurs d'adénocarcinome de côlon, MC38, allogreffées chez des souris qui ont été nourris avec une diète à haute teneur énergétique (induisant un phénotype diabétique de type II), ou un régime contrôle. Nos résultats montrent que la metformine abolie l'augmentation des niveaux sériques d'insuline, l'activation du récepteur d'insuline dans les tumeurs ainsi que l'absorption du FDG par les tumeur chez les souris ayant un régime riche en énergie et que la metformine n'a aucun effet sur ces mesures chez les souris ayant une diète contrôle. Ceci suggère que pour un sous-ensemble de néoplasmes, le régime alimentaire et le taux d'insuline influencent l'absorption du glucose par les cellules tumorales ce qui pourrait avoir une pertinence clinique dans les prochaines études clinique visant l'évaluation de l'activité anti-néoplasique de la metformine.
Shmueli, Ehoud. "Glucose metabolism and insulin resistance in cirrhosis". Thesis, University of Newcastle Upon Tyne, 1992. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.308777.
Texto completo da fonteLaberge, Marie-Kristine. "Nck1 is required for ER stress-induced insulin resistance and regulation of IRS1-dependent insulin signalling". Thesis, McGill University, 2008. http://digitool.Library.McGill.CA:80/R/?func=dbin-jump-full&object_id=111950.
Texto completo da fonteSanderson, Alison Louise. "Regulation of skeletal muscle metabolism". Thesis, University of Oxford, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.318615.
Texto completo da fonteField, Polly Ann. "The effects of insulin resistance on chylomicron metabolism". Thesis, University of Oxford, 1999. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.302120.
Texto completo da fonteDeAngelis, Anthony Michael. "CEACAM1 : a link between insulin and lipid metabolism". Connect to full text in OhioLINK ETD Center, 2009. http://rave.ohiolink.edu/etdc/view?acc%5Fnum=mco1243943993.
Texto completo da fonte"In partial fulfillment of the requirements for the degree of Doctor of Philosophy in Biomedical Sciences." Title from title page of PDF document. Bibliography: p. 57-61, p. 20-145.
Nygren, Jonas. "The sites and mechanisms of postoperative insulin resistance /". Stockholm, 1997. http://diss.kib.ki.se/1997/91-628-2695-6.
Texto completo da fonteYang, Yan. "CEACAM1: A Molecular Link Between Fat Metabolism and Insulin Clearance". University of Toledo Health Science Campus / OhioLINK, 2005. http://rave.ohiolink.edu/etdc/view?acc_num=mco1115060085.
Texto completo da fonteWang, Mengjie. "Brain Insulin-Like Growth Factor 1 Receptor and Insulin Receptor in Metabolism and Reproduction". University of Toledo Health Science Campus / OhioLINK, 2019. http://rave.ohiolink.edu/etdc/view?acc_num=mco1564676824418256.
Texto completo da fonteParpal, Santiago. "Mechanisms of insulin signaling and the role of caveolae /". Linköping : Univ, 2001. http://www.bibl.liu.se/liupubl/disp/disp2001/med684s.pdf.
Texto completo da fonteDai, Tong. "Differential Role of CEACAM Proteins in Regulating Insulin Metabolism". University of Toledo Health Science Campus / OhioLINK, 2005. http://rave.ohiolink.edu/etdc/view?acc_num=mco1139336269.
Texto completo da fonteBusquets, Figueras Oriol. "Estudi del paper de les proteïnes JNK en el desenvolupament de trastorns metabòlics i cognitius = Study on the role of the JNK proteins in the development of metabolic and cognitive disruptions". Doctoral thesis, Universitat de Barcelona, 2019. http://hdl.handle.net/10803/668381.
Texto completo da fonteMany past reports on the c-JUN N-terminal Kinases (JNKs) did not take into account the existing differences in the activity of each of the isoforms. And so, therapeutic proposals that regulated the JNKs unspecifically encountered setbacks of import. The aim of the present thesis was to contribute to current understanding of the role of individual JNK isoforms in the development of pathology and, to appraise any therapeutic interest derived of their modulation for temporal lobe epilepsy and the metabolic- cognitive syndrome. Reported results demonstrated that the knock-out JNK1 had neuroprotective effects against excitotoxic damage derived of the administration of kainic acid, a model of temporal lobe epilepsy. Thus, Licochalcone A (LIC-A), a JNK1 inhibitor, was tested for its potential as a therapeutic agent. Results confirmed that when animals were pre-treated with LIC-A they were protected from the effects of kainic acid, as demonstrated by the absence of degenerating cells and sclerotic tissue, as well as lower neuroinflammatory responses in astrocytes and microglia. Additionally, the metabolic consequences of a chronic feeding of a fat- enriched diet (High fat diet; HFD) were also assessed. Data demonstrated that HFD caused the appearance of peripheral and central insulin resistance as a result of mitochondrial and endoplasmic stress, dysregulation of autophagy and other alterations. In the end, it led to the appearance of cognitive impairments. Parallelly, the effects of the ablation of JNK2 were evaluated and, it was determined that it favoured the appearance of these same alterations, especially when combined with HFD. On the contrary, the knockout of JNK1 protected against the metabolic consequences of a chronic feeding with HFD, showing improved sensibility to insulin, reduced body weight and more efficient mitochondrial activity. Moreover, these animals were protected against the appearance of metabolic-derived cognitive dysfunctions.
Muchos estudios previos sobre el papel de las quinasas c-JUN N- terminal (JNK) no tenían en cuenta las diferencias existentes en la actividad de cada una de las isoformas. Esto provocó que las propuestas terapéuticas que regulaban las JNK de forma inespecífica se encontraran con problemas importantes. El objetivo de la presente tesis doctoral era ampliar los conocimientos que se tienen actualmente sobre el papel individual de las isoformas de las JNK y, evaluar cualquier interés terapéutico que pueda derivar de su modulación para la epilepsia del lóbulo temporal y afectaciones cognitivas derivadas del metabolismo. Estudios previos demostraron que la inactivación genética de la JNK1 tenía efectos neuroprotectores ante el daño citotóxico derivado de la administración de ácido kaínico, un modelo de epilepsia del lóbulo temporal. Por tanto, se puso a prueba el potencial terapéutico de la Licochalcona A (LIC-A), un inhibidor de la JNK1. Los resultados confirmaron que cuando los animales eran pretratados con LIC-A, estos quedaban protegidos de los efectos del ácido kaínico, tal y como lo demostraba la ausencia de células en degeneración ni de tejido esclerótico, así como una menor respuesta neuroinflamatoria en astrocitos y microglía. Además, se estudiaron las consecuencias metabólicas de una alimentación crónica con una dieta rica en grasas (HFD). Los resultados demostraban que la dieta provocaba la aparición de resistencia a la insulina a escala central y periférica como resultado de estrés en las mitocondrias y el retículo endoplasmático, desregulaciones de la autofagia, entre otros. Al final, esto llevaba a la aparición de afectaciones cognitivas. Paralelamente, se evaluaron los efectos de la inactivación genética de la JNK2 y, se determinó que favorecía la aparición de estas mismas alteraciones, especialmente cuando se combinaba con HFD. Por lo contrario, la inactivación de JNK1 protegía ante las consecuencias metabólicas de una ingesta crónica de HFD, favoreciendo una mayor sensibilidad a la insulina, un menor peso corporal y una actividad mitocondrial más eficiente. Además, estos animales quedaban protegidos ante la aparición de déficits cognitivos derivados de alteraciones metabólicas.
Dai, Tong. "Differential role of CEACAM1 and CEACAM2 in insulin metabolism". Connect to full-text via OhioLINK ETD Center, 2004. http://rave.ohiolink.edu/etdc/view?acc%5Fnum=mco1139336269.
Texto completo da fonte"In partial fulfillment of the requirements for the degree of Doctor of Philosophy in Medical Sciences." Major advisor: Sonia M. Najjar. Includes abstract. Document formatted into pages: v, 217 p. Title from title page of PDF document. Bibliography: pages 158-216.
Tan, Kathryn Choon Beng. "Postprandial lipoprotein metabolism in non-insulin-dependent diabetes mellitus". Thesis, Cardiff University, 1993. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.323795.
Texto completo da fonteAiston, Susan Michelle. "Regulation of hepatic glucose metabolism by leptin and insulin". Thesis, University of Newcastle Upon Tyne, 2001. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.341441.
Texto completo da fonteTyler-Rubinstein, Nadia. "The role of insulin receptor substrate signalling in metabolism". Thesis, Imperial College London, 2015. http://hdl.handle.net/10044/1/54894.
Texto completo da fontePotts, Jennifer Lucy. "Lipoprotein metabolism in human adipose tissue". Thesis, University of Oxford, 1993. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.334875.
Texto completo da fonteNeedham, Elise. "Personalised phosphoproteomics of skeletal muscle metabolism". Thesis, The University of Sydney, 2022. https://hdl.handle.net/2123/28191.
Texto completo da fonteStrömmer, Lisa. "Insulin action and secretion after surgical trauma : an experimental study in the rat /". Stockholm, 2001. http://diss.kib.ki.se/2001/91-628-4295-1/.
Texto completo da fonteSoop, Mattias. "Effects of perioperative nutrition on insulin action in postoperative metabolism /". Stockholm, 2003. http://diss.kib.ki.se/2003/91-7349-529-8/.
Texto completo da fonteYang, Yan. "CEACAM1 : a molecular link between fat metabolism and insulin clearance". Connect to full-text via OhioLINK ETD Center, 2004. http://rave.ohiolink.edu/etdc/view?acc%5Fnum=mco1115060085.
Texto completo da fonteIn partial fulfillment of the requirements for the degree of Doctor of Philosophy in Medical Sciences. Major advisor: Sonia Najjar. Includes abstract. Document formatted into pages: v, 167 p. Bibliography: pages 117-165.
Loos, Caroline Margot Marcelle. "THE IMPACT OF INSULIN DYSREGULATION ON PROTEIN METABOLISM IN HORSES". UKnowledge, 2018. https://uknowledge.uky.edu/animalsci_etds/83.
Texto completo da fonteCazzo, Everton 1979. "Impacto do Bypass Gastrojejunal em Y de Roux sobre a Síndrome Metabólica e seus componentes : análise de resultados". [s.n.], 2013. http://repositorio.unicamp.br/jspui/handle/REPOSIP/309054.
Texto completo da fonteDissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciências Médicas
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Resumo: A Síndrome Metabólica é um conjunto de fatores interconectados que elevam diretamente o risco de doenças cardiovasculares e diabetes mellitus tipo II. Estes fatores são alterações no metabolismo glicídico, elevação da pressão arterial, níveis elevados de triglicerídeos e reduzidos de lipoproteína de alta densidade, associados à obesidade, especialmente sua forma central ou abdominal. Apresenta prevalência crescente nas últimas décadas, levando a importantes consequências socioeconômicas. Sua fisiopatologia é complexa e ainda não foi totalmente esclarecida, porém sabe-se que possui como elemento principal a resistência insulínica. Em decorrência, observa-se a ocorrência de hiperinsulinemia, disfunção endotelial e inflamação. Seu tratamento clínico consiste em mudanças de estilo de vida associadas à terapia farmacológica concomitante de seus fatores individuais. Com a realização cada vez mais frequente de procedimentos cirúrgicos bariátricos, tem-se observado relevantes resultados advindos de tais operações no controle da síndrome. O objetivo deste estudo é avaliar o impacto do bypass gastrojejunal em Y de Roux sobre a síndrome metabólica, seus componentes individuais e as alterações bioquímicas observadas após a cirurgia. Foi realizada uma coorte histórica envolvendo 96 indivíduos com obesidade grau II/III previamente portadores de síndrome metabólica que foram submetidos à cirurgia há pelo menos 12 meses, avaliando os parâmetros clínicos e bioquímicos dos mesmos antes e após a cirurgia. Observaram-se índices relevantes de resolução pós-operatória da síndrome metabólica (88,5%), diabetes mellitus tipo II (90,6%), hipertensão arterial (85,6%) e dislipidemias (54,2%). A resolução da síndrome metabólica esteve estatisticamente associada aos seguintes fatores: controle glicêmico pós-operatório; glicemia, trigliceridemia e hemoglobinemia glicada pós-operatórias; homeostasis model assessment (HOMA) pós-operatório; número de classes anti-hipertensivas pré e pós-operatórias; percentual de perda de peso. O número de medicações anti-hipertensivas reduziu-se inclusive em indivíduos que não obtiveram resolução completa da hipertensão. Houve redução significativa nos níveis séricos de glicose, insulina, hemoglobina glicada, colesterol total, triglicerídeos e lipoproteína de baixa densidade, e elevação da lipoproteína de alta densidade. Observou-se decréscimo importante da resistência insulínica avaliada através do HOMA. Os índices de resolução de síndrome metabólica e comorbidades relacionadas encontradas neste estudo foram consistentes com achados prévios na literatura. A melhora no perfil glicêmico, insulínico e lipídico foi comparável à descrita em outros estudos, assim como a significativa redução da resistência insulínica avaliada pelo HOMA. Dentro do grupo analisado, o bypass gastrojejunal em Y de Roux apresentou resultados benéficos significativos, constituindo, portanto, uma importante ferramenta no tratamento da síndrome metabólica, propiciando elevados índices de resolução da mesma e de seus componentes individuais, bem como melhora geral do perfil bioquímico relativo à patologia
Abstract: Metabolic syndrome is defined as a set of interconnected factors that increase risk for cardiovascular disease and type II diabetes. These factors are changes on glycemic metabolism, high blood pressure, high serum triglyceride levels and low high density lipoprotein serum levels, associated with obesity, specially the central or abdominal type. Its prevalence has raised on later decades leading to important socioeconomical consequences. It has a complex pathophysiology that has not been completely understood yet but it is known that its main element is insulin resistance. As consequence it is observed hyperinsulinemia, endothelial disfunction and inflammation. Clinical management is based on lifestyle changes associated to drug treatment of its individual components. As surgical treatment of obesity has become more frequent lately it has been seen great results on metabolic syndrome control after bariatric procedures. This study aims to determine the impact of Roux-en-Y gastric bypass on metabolic syndrome and its individual components as well as biochemical changes upon glycemic metabolism observed after surgery. A historic cohort was carried out evaluating 96 subjects with grade II/III obesity previously diagnosed with metabolic syndrome who underwent surgery and whose postoperative follow-up was at least 12 months. Clinical and biochemical parameters were analyzed before and after surgery. This study has shown high resolution rates of metabolic syndrome (88,5%), diabetes (90,6%), hypertension (85,6%) and dyslipidemias (54,2%). Metabolic syndrome resolution was statistically linked to these factors: postoperative glycemic control; postoperative glycemia, hemoglobin A1c and triglyceridemia; postoperative homoestasis model assessment (HOMA); pre and postoperative number of anti-hypertensive classes; percent weight loss. Number of anti-hypertensive classes decreased even in subjects who do not achieve complete hypertension resolution. There was significant decrease on serum levels of glucose, insulin, hemoglobin A1c, total cholesterol, triglycerides and low density lipoprotein, and increase on high density lipoprotein. It was observed relevant decrease on insulin resistance assessed through HOMA. Resolution rates for metabolic syndrome and related comorbidities found on this study were comparable to previous findings on medical literature. Improvement on glycemic, insulinic and lipid profiles was also similar to previous findings, as well as significant decrease on insulin resistance as evaluated through HOMA. Within this group of subjects Roux-en-Y gastric bypass has led to significant positive results proving to be an important therapeutical tool on metabolic syndrome management since it can bring high resolution rates of the syndrome and its individual components as well as general improvement on the biochemical profile related to this pathology
Mestrado
Fisiopatologia Cirúrgica
Mestre em Ciências
Rincón, Viatela Jorge E. "Regulation of glucose transport and insulin-stimulated glut4 translocation in skeletal muscle /". Stockholm, 1998. http://diss.kib.ki.se/1998/91-628-3297-2/.
Texto completo da fonteKamel, Ashraf Fawzy. "Insulin and growth hormone : regulation of adipocyte metabolism during infancy and childhood /". Stockholm, 1999. http://diss.kib.ki.se/1999/91-628-3485-1/.
Texto completo da fonteOsei, Michael. "A study of dietary fat metabolism in healthy and insulin resistant subjects". Thesis, University of Cambridge, 2015. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.708531.
Texto completo da fonteReis, Sabrina Karen 1989. "Efeitos da suplementação com l-glutamina nos níveis séricos de hormônios relacionados ao metabolismo energético em indivíduos com sobrepeso e obesidade". [s.n.], 2014. http://repositorio.unicamp.br/jspui/handle/REPOSIP/244476.
Texto completo da fonteDissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciências Aplicadas
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Resumo: Obesidade está associada à inflamação crônica de baixo grau e ao desenvolvimento da resistência à insulina. A suplementação com L-glutamina tem sido utilizada para reduzir a inflamação em pacientes críticos. No entanto, os efeitos da suplementação deste aminoácido em doenças inflamatórias de baixo grau, como a obesidade, ainda não foram investigados. Por tanto o objetivo do presente estudo foi investigar se a suplementação oral com L-glutamina altera a massa corporal, circunferência da cintura, sensibilidade à insulina e os níveis séricos de hormônios relacionados ao metabolismo energético em indivíduos com sobrepeso e obesidade. Foi realizado um estudo clínico randomizado, simples cego com 67 voluntários adultos do Hospital Estadual de Sumaré (HES), classificados com sobrepeso (IMC 25 a 29,9 kg/m²) ou obesidade (IMC ? 30). Os indivíduos foram suplementados com 30 g/dia de glutamina ou alanina durante 14 dias. Os níveis séricos de insulina, leptina, adiponectina e GLP-1 foram avaliados no período pré e pós-suplementação, pelo método de ELISA. A glicose sérica foi avaliada pelo método da glicose oxidase. O índice de HOMA foi calculado. A massa corporal, o índice de massa corporal (IMC), a circunferência da cintura e o recordatório alimentar de 24 horas, também, foram avaliados pré e pós-suplementação. A suplementação oral com L-glutamina não alterou a massa corpórea e o IMC, no entanto reduziu a circunferência da cintura e os níveis séricos de leptina, sugerindo uma diminuição na massa adiposa. Não houve diferença significativa nos níveis séricos de glicose, adiponectina e GLP-1. Entretanto, houve uma redução nos níveis séricos de insulina e índice de HOMA, sugerindo uma redução na inflamação de baixo grau e uma melhora na sensibilidade à insulina. Os dados obtidos sugerem que a suplementação oral com L-glutamina em um curto período de tempo pode reduzir a massa adiposa de indivíduos com sobrepeso e obesidade. Essa redução refletiu nos níveis séricos de leptina e provavelmente nos níveis séricos de insulina, melhorando a sensibilidade à insulina. Por tanto, a suplementação com L-glutamina pode tornar-se uma abordagem terapêutica interessante para os indivíduos com sobrepeso e obesidade
Abstract: Obesity is associated with low-grade inflammation and insulin resistance. Glutamine supplementation has been used to reduce inflammation in critically ill patients. However, the effects of glutamine supplementation were not yet investigated in diseases with lowgrade inflammation such as obesity. Previous data showed that glutamine supplementation reduced inflammation, adipose mass and improved insulin sensitivity of obese rats. Thus, the aim of this study was to investigate whether oral glutamine supplementation alters body weight (BW), waist circumference (WC) and hormones levels and insulin sensitivity in overweight and obese humans. A randomized clinical trial, single blind with 67 adult volunteers from the State Hospital of Sumaré (HES), classified as being overweight (IMC 25 a 29,9 kg/m²) or obese (IMC ? 30) was performed. The subjects were supplemented with 30 g / day glutamine or alanine for 14 days. Serum levels of insulin, leptin, adiponectin and GLP-1 were evaluated before and after supplementation, by ELISA. Serum glucose was measured by glucose oxidase method. The HOMA index was calculated. The body weight, body mass index (BMI), waist circumference and 24-hour food record were also evaluated before and after supplementation. Glutamine supplementation did not change BW and BMI, however, reduced WC and serum leptin levels, suggesting a decrease in fat mass. Glutamine supplementation l did not alter serum adiponectin, GLP-1 and glucose levels. However, was reduced insulin levels and HOMA index, suggesting a reduction in low-grade inflammation associated with an improvement of insulin sensitivity. The data suggest that oral supplementation with L-glutamine in a short period of time can reduce fat mass in overweight and obese individuals. This reduction reflected in serum leptin levels and probably in serum insulin levels, improving insulin sensitivity. Thus, glutamine supplementation may become an interesting therapeutic approach for individuals with overweight and obesity
Mestrado
Nutrição
Mestra em Ciências da Nutrição e do Esporte e Metabolismo
Gil, Paulo César Nunes. "Uso da maltodextrina na substituição do amido em dieta para eqüinos". Universidade de São Paulo, 2010. http://www.teses.usp.br/teses/disponiveis/10/10135/tde-21092010-133608/.
Texto completo da fonteThe objective of this study was to determine the effects of supplementation with maltodextrin, the replacement of starch in the diet of horses by evaluating the apparent digestibility of dry matter and nutrient and differences in glycemic responses and insulinemic certain diets. There were four female horses aged approximately 30 months, average weight of 400 kg, belonging to the flock of USP. The animals were immunized against tetanus, wormed and pulverized against ectoparasites. The diet was composed by 50% concentrate and 50% forage diet formulated to meet the demands of growth and maintenance of category equine use. The diets contained 50% starch in the concentrate, replaced in 33, 66 and 100% of maltodextrin. The total collection of feces was made in a period of 24 hours over 03 (three) days, with animals kept in stalls with concrete floor, without bedding. On the first day of faeces were carried out blood samples in tubes previously prepared with stabilizers from the jugular vein 30 minutes before 30 minutes, 90 minutes, 150 minutes, 210 minutes after delivery of the concentrate to measure glucose and insulin. Were not observed effects linear or quadratic for the coefficients of apparent digestibility of dry matter and nutrient, however it was observed a higher coefficient of apparent digestibility of the ration with 100% replacement of starch by maltodextrin in concentrated, dry matter, organic matter, crude protein, neutral detergent fiber and acid. For the glycemic responses and insulin levels were observed quadratic effect for glucose when we analyzed the area under the curve of this variable. Similarly, it was observed a linear behavior for insulin. When analyzing their response as a function of time was observed a peak of glucose and insulin between the time of 1.5 to 2 hours post-feeding in relation to glucose diet with 66% replacement had a higher peak and cooperation with 100% replacement had a higher peak insulin. The results of maltodextrin use on digestive physiology and its post prandial behavior in equines allow its inclusion in animal diets.
Lemley, Caleb Owens. "Alterations in progesterone catabolic enzymes by insulin". Morgantown, W. Va. : [West Virginia University Libraries], 2007. https://eidr.wvu.edu/etd/documentdata.eTD?documentid=5286.
Texto completo da fonteNesin, April Erwin. "Relationship between Emotional Competence and Metabolic Control in Adolescents with Insulin Dependent Diabetes Mellitus (IDDM)". Fogler Library, University of Maine, 2004. http://www.library.umaine.edu/theses/pdf/NesinAE2004.pdf.
Texto completo da fonteIsaksson, Bengt. "Insulin resistance in pancreatic cancer /". Stockholm, 2003. http://diss.kib.ki.se/2003/91-7349-493-3/.
Texto completo da fonteYamamoto, Daniel L. "Adrenergic signaling in insulin-sensitive tissues". Doctoral thesis, Stockholm : Wenner-Gren Institute for Experimental Biology, Stockholm University, 2007. http://urn.kb.se/resolve?urn=urn:nbn:se:su:diva-6668.
Texto completo da fonteForbes, Johnathon. "Hormonal Regulation of Glucose Kinetics in Rainbow Trout: Effects of Insulin and Glucagon". Thesis, Université d'Ottawa / University of Ottawa, 2019. http://hdl.handle.net/10393/39050.
Texto completo da fonteKim, Tae-gyu. "Effects of #beta#-casomorphins on metabolism of dairy cows". Thesis, University of Glasgow, 1999. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.301620.
Texto completo da fonteCambron, Liz Doralyn. "Factors Affecting Metabolism During Non-Feeding Stages in Insects". Diss., North Dakota State University, 2020. https://hdl.handle.net/10365/31868.
Texto completo da fonteBevan, Samantha J. "Factors influencing the sensitivity of skeletal muscle glucose metabolism to insulin". Thesis, University of Oxford, 1992. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.305419.
Texto completo da fonteGlynn, M. J. "The implications of insulin and protein metabolism for clinical nutritional support". Thesis, University of Cambridge, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.599445.
Texto completo da fonteKapan, Neval. "Regulation of insulin producing cells, stress responses and metabolism in Drosophila". Doctoral thesis, Stockholms universitet, Zoologiska institutionen, 2012. http://urn.kb.se/resolve?urn=urn:nbn:se:su:diva-80518.
Texto completo da fonteAt the time of the doctoral defense, the following paper was unpublished and had a status as follows: Paper 3: Epub ahead of print. Paper 4: Manuscript.
Sweeney, Gary. "Protein kinase C isoforms : insulin signalling, cyclic amp metabolism and diabetes". Thesis, University of Glasgow, 1994. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.306884.
Texto completo da fontePennington, S. R. "The effects of insulin on phosphoinositide metabolism in isolated fat cells". Thesis, University of Cambridge, 1986. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.382660.
Texto completo da fonteNixon, Mark. "Interactions between glucocorticoid metabolism and inflammation in obesity and insulin resistance". Thesis, University of Edinburgh, 2011. http://hdl.handle.net/1842/5593.
Texto completo da fonteDean, John Duncan. "Lipoprotein metabolism and macrovascular disease in non-insulin dependent diabetes mellitus". Thesis, University of Leicester, 1993. http://hdl.handle.net/2381/34322.
Texto completo da fonteGomez, Cristina Alexandra Silva. "Tratamento ortodôntico em pacientes diabéticos". Master's thesis, [s.n.], 2015. http://hdl.handle.net/10284/4748.
Texto completo da fonteA diabetes mellitus é um síndrome ou distúrbio na homeostase da glicose causada por uma deficiência de insulina ou por uma ação anormal desta no metabolismo de hidratos de carbono, proteínas e gordura. É a desordem endrocrino-metabólica mais comum na infância e adolescência, com consequências no desenvolvimento físico e emocional dos seus portadores. (Meyle et alii, 2001) O objetivo do presente trabalho é caracterizar o paciente diabético, reconhecendo as suas características particulares, limitações e possíveis complicações e relacioná-lo com o tratamento ortodôntico, referindo as alterações orais que um paciente diabético pode apresentar aquando do tratamento; para além disto, é também focada a importância da saúde periodontal para estes pacientes, pois esta, juntamente com o bom controlo metabólico da doença, permite a realização do tratamento ortodôntico em condições favoráveis. A realização desta Monografia insere-se no Mestrado Integrado em Medicina Dentária e tem como base um estudo de literatura científica nas áreas da Biologia, Anatomia, Medicina e Ortodontia, tendo sido utilizados diversos motores de busca para o efeito. Diabetes mellitus is a syndrome or disturb in the glucose homeostasis, caused by a insulin deficiency or by a abnormal action of this hormone in the carbohidrates, protein and fat metabolism. It’s the most common endocrine-metabolic disease in childhood and adolescence, which has several consequences in the physical and psychological development of those who have it. (Meyle et alii, 2001) The purpose of this work is to characterize the diabetic patient, recognizing its particular characteristics, limitations and possible complications, and relate it with and orthodontic treatment, presenting as well the oral alterations that this patients can present at the time of the orthodontic treatment; it is as well refered the importance of periodontal health to this patients because this, combined with a good metabolic control, allows the realization of the treatment in good conditions. This monography was undertaken within the Master in Dental Medicine and was based in a scientific literature study based os areas such as Biology, Anatomy, Medicine and Orthodontics.
Oliveira, Neto Jessika Geisebel. "Impacto da suplementação materna com extrato aquoso de canela durante a lactação sobre a homeostase energética da prole adulta". Niterói, 2017. https://app.uff.br/riuff/handle/1/3779.
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A programação metabólica ocorre quando insultos promovem alterações adaptativas nos períodos críticos do desenvolvimento e alteram as funções endócrino-metabólicas ao longa da vida. Estudos com alimentos conhecidos por trazerem benefícios à saúde além do valor nutritivo, mostraram que seu consumo por mães gestantes e/ou lactantes podem vir a ter desfechos negativos para a prole. Já está bem caracterizado que a ingestão de canela gera benefícios para homeostase energética. Entretanto, dados prévios obtidos pelo grupo mostraram que a suplementação com extrato aquoso de canela (400mg/kg peso corporal/dia) durante a lactação leva ao desenvolvimento de obesidade visceral, hiperleptinemia, hiperinsulinemia, associada a normoglicemia, na prole adulta aos 180 dias de vida. Com o objetivo de melhor compreender as alterações endócrino-metabólicas deste modelo, avaliamos a expressão proteica no fígado e músculo esquelético por Western blot, além de avaliarmos o conteúdo de triglicerídeo e glicogênio hepáticos através de ensaios colorimétricos. No fígado, vimos uma diminuição na fosforilação do IR, entretanto, observamos aumento na fosforilação do IRS1 e AKT. Quando avaliamos a sinalização de leptina, não observamos alteração na expressão do ObRB e SOCS3, no entanto, vimos um aumento na expressão da JAK2 e na fosforilação da STAT3, sugerindo que a ativação do IRS1/AKT possa decorrer da maior ativação da via da leptina. Apesar de não observarmos alteração da via gliconeogênica (PEPCK, G6Pase, GLUT2), vimos que a programação leva a um menor conteúdo de glicogênio hepático acompanhado por maior ativação da GSK3β. Observamos aumento do conteúdo de triglicerídeo hepático acompanhado por expressão normal do PPARα e uma interessante redução da expressão do SREBP1c. Concluímos que a programação por canela na lactação altera as principais ações da insulina no fígado, levando a uma menor síntese de glicogênio e acúmulo de gordura neste tecido, sem gerar alterações significativas no músculo esquelético.
Metabolic programming occurs when insults promotes adaptive changes in critic periods of development that alters the endocrine-metabolic functions in the offspring in medium and long terms. Studies with foods known to promote health benefits in addition to the nutritive value, shows that its consumption by pregnant and/or lactating females could induce negative outcomes to the offspring. It is well characterized that cinnamon intake promotes benefits to energy homeostasis. However, previous data obtained by our research group showed that supplementation with cinnamon water extract (400mg/kg body weight/day) during lactation leads to the development of visceral obesity, hyperleptinemia, hyperinsulinemia, associated to normoglycemia, in the adult offspring with 180 days old. To increase the knowledge about the endocrine-metabolic changes in this model, we evaluated the protein expression in liver and skeletal muscle by Western blot, and evaluated the hepatic content of triacylglycerol and glycogen using colorimetric assays. In liver, we observed a reduced IR phosphorylation; however, we observed increased phosphorylation of IRS1 and AKT. Concerning leptin signaling pathway, we did not observed changes in the ObRB and SOCS3 expression, but we observed an increased expression of JAK2 and phosphorylation of STAT3, suggesting that the activation of IRS1/AKT could be resulted by the increased activation of leptin signaling pathway. Although we observed no changes in the gluconeogenic pathway (PEPCK, G6Pase, GLUT2), we observed that the programmed group exhibit a lower hepatic glycogen content accompanied by increased activation of GSK3β. We observed increased hepatic triacylglycerol content accompanied by normal PPARα expression and an interesting reduction of SREBP1c expression. We conclude that the programming induced by cinnamon intake during lactation alters the main actions of insulin in liver; leading to lower glycogen synthesis and accumulation of fat in this tissue, without promote important changes in skeletal muscle.
Crawford, Lynne Mary. "The regulation of triglyceride metabolism in the liver and adipose tissue". Thesis, University of Glasgow, 1998. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.263457.
Texto completo da fontePenteado, Érica 1973. "Tratamento com topiramato melhora a sensibilidade hipotalâmica à insulina em camundongos obesos". [s.n.], 2011. http://repositorio.unicamp.br/jspui/handle/REPOSIP/311559.
Texto completo da fonteDissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciências Médicas
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Resumo: O topiramato (TPM) é utilizado atualmente no tratamento da epilepsia e da enxaqueca por ser antagonista do receptor AMPA/KA e por aumentar o receptor de GABA, desencadeando a estabilização dos canais de sódio e cálcio. O efeito colateral mais conhecido dessa droga é a perda de peso, o aumento do gasto energético e da termogênese. Os hormônios anorexigênicos insulina e leptina regulam a atividade de populações distintas de neurônios que controlam o balanço energético via ativação da via IR/PI3K/Akt e OBR/JAK2/STAT3 respectivamente. Entretanto, desconhece-se se o efeito do TPM na perda de peso é decorrente de alterações da ação insulínica ou de leptina no hipotálamo. Assim, o objetivo do estudo é investigar se o tratamento com essa droga altera a sinalização da insulina e da leptina em hipotálamo de camundongos alimentados com dieta hiperlipídica (DH) ou ração padrão. Camundongos Swiss obesos ou com dieta padrão foram submetidos à cirurgia estereotáxica para inserção de cânula no ventrículo lateral. Após uma semana de recuperação, as cânulas foram testadas, e os animais foram tratados com 110mg/kg/dia de TPM, via gavagem, por sete dias, tendo sua ingestão alimentar e peso corpóreo monitorados diariamente. Observou-se que os animais em DH, tratados com TPM, possuem um menor ganho de peso e de ingestão alimentar do que seus controles, tratados com veículo. Não houve, porém, diferença quanto ao ganho de peso e ingestão alimentar dos animais tratados com a droga não obesos. Observou-se um aumento da termogênese nos animais obesos tratados com TPM pelo aumento da expressão da proteína UCP1, proteína desacopladora mitocondrial do tecido adiposo marrom, e também pelo aumento do consumo de O2 e produção de CO2, marcadores de termogênese. A nível molecular, os animais obesos apresentaram redução da fosforilação do receptor de insulina, IRS-1 e Akt induzidos por insulina e redução da fosforilação de OBR/JAK2/STAT3 induzida por leptina em hipotálamo. Entretanto, o tratamento com TPM reverteu este efeito, sugerindo que o tratamento com a droga induz uma melhora da ação/sinalização insulínica e de leptina no hipotálamo de camundongos obesos. Dessa maneira, sugere-se que o tratamento com TPM, pelo menos a curto prazo, melhora da ação e sinalização da insulina e leptina em hipotálamo, podendo ser um dos mecanismos pelos quais ocorre redução da ingestão alimentar e aumento do gasto energético nesses animais. Essa alteração de ingestão e de termogênese pode contribuir para a redução da adiposidade de camundongos obesos tratados com topiramato. Assim, essa droga parece ter um potencial terapêutico no tratamento da obesidade e da resistência à insulina
Abstract: Topiramate (TPM) is an anticonvulsant drug used for the treatment of epilepsy and prophylaxis of migraine. Weight loss is a frequently side effect reported in patients and animal models treated with TPM. In animal models topiramate may increase levels of hypothalamic corticotropic-releasing hormone (CRH), which is an anorexigenic neuropeptide and may decrease food intake. Some studies showed that topiramate may decrease energy storage, and thus increase energy expenditure and thermogenesis. However, the mechanisms by which TPM reduces body weight are not completely known so far. The hypothalamus is acknowledged as an important regulator of whole-body energy homeostasis by integrating nutrient and hormones signals from central and peripheral inputs. Anorexigenic hormones such as insulin and leptin regulate the activity of distinct neuron populations that control energy balance via IR/PI3K/Akt/Foxo1 pathway or OBR/JAK2/STAT3 pathway respectively. However, if topiramate alters hypothalamic insulin or leptin sensitivity is not known. Thus, in the present study, we asked whether topiramate treatment alters energy balance by altering insulin and leptin action/signaling in the hypothalamus from control and diet-induced obesity (DIO) mice. Our data provide evidence that short treatment with topiramate improves hypothalamic insulin and leptin signaling and action in obese mice. The improvement of hypothalamic insulin and leptin may reduce food ingestion and increase energy expenditure by increases in CRH and TRH mRNA expression. The lower food intake and higher energy expenditure induced by topiramate treatment may reduce obesity in mice on high fat feeding and may be an alternative therapy for obese treatment
Mestrado
Ciencias Basicas
Mestre em Clinica Medica
Frias, Flávia de Toledo. "Papel dos microRNAs (miR-1, miR-133, miR-206, miR-208b, miR-499 e miR-223) no músculo esquelético de camundongos C57BL/6 durante o estado de resistência à insulina". Universidade de São Paulo, 2016. http://www.teses.usp.br/teses/disponiveis/42/42136/tde-12092016-085246/.
Texto completo da fonteIn skeletal muscle (SM) tissue, evidences suggest that the high availability of free fatty acids (FFAs) observed in obesity plays a central role in the development of insulin resistance (IR) by causing changes in mitochondrial function. Since microRNAs (miRs) are recently identified molecules acting as gene regulators of metabolic pathways, we aimed to investigate in SM of insulin resistant mice induced by 8 weeks of high-fat diet (HFD) feeding, treated with fenofibrate (CF and HF) or metilcelulose (vehicle, C and H) two weeks before euthanasia, if miRs-1a, 133a/b, 206, 208b, 499 and 223 are involved in IR pathogenesis. IR was induced after 8 weeks of HFD (H), and fenofibrate treatment (HF) partially reverted this condition by causing alterations on metabolic and enzymatic parameters, which seems to be mediated by miR-1a regulating AMPKα2 protein. AMPKα2 increased translation active catabolic processes such as glucose uptake and FFAs oxidation, being considered the main regulator of cell metabolism by stimulating mitochondrial genes expression via PGC-1α.