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31	Rôle du stress oxydant en période néonatale dans l'hypertension artérielle et la dysfonction vasculaire et métabolique de l'adulte Yzydorczyk, Catherine 01 1900 (has links) Introduction De nombreuses études indiquent que la prématurité, qui représente 8 % des naissances, est associée à des indices précoces de dysfonction vasculaire, d’élévation de la pression sanguine et de survenue de diabète de type 2. Les enfants nés prématurément sont plus sujets aux blessures oxydatives de par l’immaturité de leurs défenses antioxydantes et de leur exposition à des situations pro-oxydantes (exposition à l’air ambiant, à un supplément d’oxygène, ou à une exposition aux infections). Cependant, les conséquences à long terme des blessures oxydatives induites par une exposition à l’oxygène en période périnatale restent méconnues. Le but de ce doctorat a été de mettre en évidence certains mécanismes pouvant relier les dommages de la prématurité induits par l’oxygène, et le risque à long terme de développer des maladies cardiovasculaires et métaboliques dans le concept global d’une programmation développementale de l’hypertension et des pathologies reliées au syndrome métabolique. Matériels et méthodes Des ratons Sprague-Dawley (SD) ont été exposés à 80 % O2 (O2) vs air ambiant (AA) du 3ème au 10ème jour de vie. Concernant les paramètres cardiovasculaires, nous avons mesuré au cours de la croissance, la pression sanguine à la queue (de la 4ème semaine à la 15ème semaine) et à l’âge adulte : la réactivité vasculaire à l’angiotensine II (AngII) et au carbachol (ex vivo, carotides) avec ou sans le tempol; la production d’oxyde nitrique (NO) en présence ou non L-arginine et de L-sépiaptérine (aorte, immunohistochimie) ainsi que l’expression de la nitric oxyde synthase endothéliale (eNOS) (aorte, immunohistochimie et western blot); le stress oxydant vasculaire (aorte, chemiluminescence) par la mesure de la production d’anions superoxide en présence ou non des inhibiteurs de la nicotinamide-adenine-dinucleotide-phosphate (NADPH oxydase) et de la nitric oxyde synthase endotheliale (eNOS), l’apocynine, et N-nitro-L-arginine methyl ester (L-NAME) respectivement, ainsi que le stress oxydant circulant par la mesure des niveaux plasmatiques de malondialdéhyde (MDA, HPLC); la densité microvasculaire a été évaluée au niveau du muscle tibial antérieur, immunohistochimie); la vitesse d’onde pulsée (VOP) (entre la valve aortique et juste avant la bifurcation ilio-fémorale) a été mesurée par ultrason; le nombre de néphrons a été compté par digestion acide. L’ontogenèse de la plupart de ces mécanismes a été regardée à l’âge de 4 semaines. Concernant les paramètres métaboliques, le poids a été mesuré au cours de la croissance. À l’âge adulte, la composition corporelle et la tolérance au glucose ont été évaluées. Résultats À l’âge de 4 semaines, aucune différence n’a été observée dans la pression sanguine, la réactivité vasculaire et le stress oxydant, mais chez les rats O2 vs AA, la densité microvasculaire est moindre, et des changements histologiques suggèrent la présence d’une rigidité artérielle augmentée. À l’âge adulte chez les rats O2 vs AA (n = 6-8 /groupe) : i) les pressions sanguines systoliques et diastoliques sont augmentées; ii) la réactivité vasculaire à l’AngII est augmentée et celle au carbachol est diminuée, le tempol prévient ces dysfonctions; iii) la production de NO est plus faible au niveau basal et après stimulation par le carbachol, mais est restaurée après la pré-incubation avec L-arginine et L-sépiaptérine; iv) l’expression d’eNOS est diminuée par immunohistochimie et augmentée par western blot; v) les niveaux d’anions superoxide, au niveau basal et en réponse à l’AngII, sont augmentés et sont induits par la NADPH oxydase et le non-couplage d’eNOS; vi) les niveaux plasmatiques de MDA sont augmentés; vii) La densité microvasculaire est moindre; viii) la VOP est augmentée; ix) le nombre de néphrons par rein est réduit; x) le poids est plus faible au cours de la croissance et un catch up est observé à l’âge adulte; la composition corporelle n’est pas différente entre les groupes; xi) la tolérance au glucose est diminuée. Conclusion Ces résultats supportent l’hypothèse d’une programmation développementale des maladies cardiovasculaires et métaboliques à l’âge adulte à la suite d’un stress hyperoxique néonatal. / Introduction Many studies showed that prematurity, which represents 8 % of birth, is associated with early indices of vascular dysfunction, increased blood pressure and Type 2 diabetes. Prematurity babies are more susceptible to oxidative injury, consequence of the immaturity of their antioxidant defences, and exposure to pro-oxidant situations (oxygen supplementation, infection). However, the long-term consequences of oxidative injury induced by oxygen exposure in the neonatal period are unknown. The aim of these PhD studies was to unravel some mechanisms that might underlie the damage induced by oxygen and the long-term risk of developing vascular and metabolic diseases in the overall concept of developmental programming of hypertension and metabolic syndrome-related diseases. Materials and methods Sprague-Dawley pups were kept with their mother in 80 % O2 (O2) or room air (RA) from day 3 to 10 of life. Cardiovascular parameters, tail blood pressure was measured between 4 and 15 weeks of life. In adulthood : vascular reactivity (ex vivo carotid rings) to angiotensine II (AngII) and carbachol with and without tempol was studied; studies of nitric oxide (NO) production with and without L-arginine and L-sépiaptérine (aorta, immunohistochemistry) and endothelial nitric oxide synthase expression (eNOS; aorta, immunohistochemistry, western blot) were performed; vascular oxidative stress (aorta, using chemiluminescence) by measuring superoxide anion production with and without inhibitors of nicotinamide-adenine-dinucleotide-phosphate (NADPH oxydase) and nitric oxyde synthase endotheliale (eNOS), apocynin and N-nitro-L-arginine methyl ester (L-NAME) respectively, and circulating oxidative stress by measuring the plasma levels of malondialdéhyde (MDA, HPLC) were evaluated; microvascular density was assessed on tibialis anterior muscle sections; pulse wave velocity (PWV) was measured by ultrasound, between aortic valve and ilio-femoral bifurcation; nephrons were counted after hydrochloric acid digestion. The main observations were also evaluated at 4 weeks of age. Metabolic parameters: body weight has been measured during the growth. In adulthood, body composition, glucose tolerance were evaluated. Results A 4 weeks of age, no difference was observed regarding blood pressure, vascular reactivity, and oxidative stress indices, but in rats O2 vs. RA (n = 6-8 /group), microvascular rarefaction and histological changes suggesting enhanced vascular stiffness were present. To adulthood, rats O2 vs. RA (n = 6-8/group) : i) systolic and diastolic blood pressures are increased; ii) vascular reactivity to Ang II is increased and to carbachol is decreased, these dysfunction were totally abolished by co-incubation of the vessel rings with tempol; iii) NO-production is decreased in basal condition and after carbachol stimulation, but is restored after pre-incubation of aorta sections with L- arginine and L-sépiaptérine; iv) eNOS expression is decreased by immunohistochemistry but increased by western blot; v) vascular superoxide anion levels are increased in basal condition, after AngII stimulation and this is mediated by NADPH oxydase and eNOS uncoupling; vi) the plasma levels of MDA are increased; vii) microvascular density is decreased; viii) PWV is increased; ix) nephron count per kidney is decreased; x) body weight is less during growth, but a catch up is observed in adulthood, body composition is similar; xi) the glucose tolerance is decreased in adults. Conclusion These results support the hypothesis of developmental programming of vascular and metabolic diseases in adulthood, after exposure to hyperoxic stress in the neonatal period. / Thèse réalisée dans le cadre d'une cotutelle entre l'Université de Montréal et l'Université d'Auvergne en France hypertension hypertension réactivité vasculaire vascular reactivity stress oxydant oxidative stress intolérance au glucose glucose intolerance résistance à l'insuline insuline resistance syndrome métabolique metabolic syndrome
32	Innate Immunity in Type 2 Diabetes Pathogenesis: Role of the Lipopolysaccharide Signaling Cascade: A Dissertation Young, James L. 01 July 2008 (has links) Once seen as a disease of wealthy nations, type 2 diabetes mellitus is now showing unprecedented growth throughout the world, fueling increases in microvascular and macrovascular complications. A compelling and growing body of evidence suggests that glucose intolerance and insulin resistance, hallmarks of the diabetic patient, may be driven by chronic inflammation. In particular, a predominance of visceral fat has been associated with enhanced inflammatory cytokine secretion that may contribute to enhanced risk of diabetes and comorbid cardiovascular disease in these individuals. As a function of its potency and wide environmental and biological distribution, we hypothesized that bacterial lipopolysaccharide (LPS, also known as endotoxin) may promote adipose inflammation and concomitant metabolic dysfunction. Indeed, expression of the LPS receptor CD14 is enhanced on visceral adipocytes of ob/ob mice, paralleling enhanced IL-6 secretion ex vivo. Furthermore, rosiglitazonefed ob/obmice demonstrated a reduction in CD14 that coordinated with diminished IL-6 secretion, suggesting a basis for the touted anti-inflammatory effects of this commonly employed type 2 diabetes medication. Mice deficient in components of the LPS signaling cascade, namely CD14, TLR4, and MyD88, yielded adipocytes with markedly attenuated IL-6 secretion, corroborating the central importance of LPS in adipocyte inflammation and supporting the role of this signaling pathway in depot-specific inflammation. Despite the prominent role of LPS signaling in adipocyte inflammation, CD14-, TLR4-, and MyD88-deficient mice failed to show resistance to diet induced obesity. Surprisingly, cd14-/- and tlr4-/- mice had marked glucose intolerance without alteration in total weight or adipose accumulation. In contrast, myd88-/- mice revealed minor glucose intolerance only with high fat diet challenge at an advanced age despite being overtly obese. In cd14-/- and tlr4-/-, but not myd88-/-, mice, an exaggerated rebound to hypoglycemia was associated with enhanced norepinephrine secretion, which could be abrogated by the adrenergic β-blocker propranolol. The overlay of these mouse models reveals a divergence of phenotypes that demonstrate LPS signaling disruption may lead to glucose intolerance and insulin resistance in part due to enhanced sympathoadrenal tone, uncovering an essential role of innate immunity in physiological stress and its impact upon glucose homeostasis. Diabetes Mellitus Type 2 Lipopolysaccharides Antigens CD14 Inflammation Adipocytes Insulin Resistance Glucose Intolerance Mice Amino Acids, Peptides, and Proteins Animal Experimentation and Research Biological Factors Carbohydrates Endocrine System Diseases Nutritional and Metabolic Diseases
33	Glicemia de jejum, diabetes incidente, aterosclerose subclínica e eventos cardiovasculares não-fatais numa amostra de adultos aparentemente saudáveis reavaliados após 12 anos / Fasting plasma glucose, incident diabetes, subclinical atherosclerosis and non-fatal cardiovascular events in an apparently healthy adult sample reevaluated after a 12 years interval Sitnik, Debora 01 November 2016 (has links) Introdução: Glicemia de jejum alterada tem sido associada a maior risco de desenvolver diabetes, comparando a indivíduos normoglicêmicos. Apesar de diabetes ser relacionado a aterosclerose e a piores desfechos cardiovasculares, os dados de literatura relacionando glicemia de jejum alterada à doença aterosclerótica são conflitantes. Os objetivos deste trabalho foram determinar (a) a incidência de diabetes em indivíduos com glicemia de jejum normal ou alterada em 1998 após um seguimento de até 12 anos; (b) se a glicemia de jejum alterada em 1998 e/ou diabetes incidente estiveram associados com aterosclerose subclínica no Estudo Longitudinal da Saúde do Adulto (ELSA-Brasil) ou à variável combinada de eventos clínicos não-fatais e escore de cálcio coronariano maior ou igual a 400. Métodos: Avaliamos 1.536 trabalhadores da Universidade de São Paulo, que participaram de um programa de avaliação em 1998 (idade 23-63 anos) e da linha de base do ELSA-Brasil (2008-2010). Apresentamos as taxas de incidência de diabetes brutas e ajustadas para todos os indivíduos e também estratificados por gênero e por índice de massa corpórea (IMC) em 1998. Utilizamos modelos de regressão brutos e ajustados para estimar a associação entre glicemia de jejum alterada em 1998 ou diabetes incidente com a espessura de íntima-média de carótidas (EIMC), escore de cálcio coronariano (CACS, do inglês Coronary Artery Calcium Score) e a variável composta CACS >= 400 ou eventos cardiovasculares incidentes (infarto do miocárdio ou revascularização). Resultados: Encontramos diabetes incidente em 177 indivíduos. A incidência de diabetes em nossa amostra foi de 9,8/1.000 pessoas-ano (Intervalo de confiança de 95% [IC95%]: 7,7-13,6). A incidência foi mais elevada entre os homens (11,2/1.000 pessoas-ano, IC95%: 8,6-15,0) do que entre as mulheres (8,5/1.000 pessoas-ano, IC95%: 5,3-15,3). Glicemia de jejum alterada em 1998 mostrou associação com maior risco de progressão para diabetes ao longo do seguimento (hazard ratio [HR]: 3,17; IC95%: 2,14-4,68) e HR: 7,42; IC95%: 4,75-11,57 para glicemias de jejum entre 100 e 109mg/dl e entre 110 e 125mg/dl, respectivamente). Glicemias entre 110 e 125mg/dl em 1998 foram associadas a maiores valores de EIMC (beta=+0,028; IC95%: 0,003 a 0,053) na linha de base do ELSA-Brasil. Ao excluir da análise aqueles com diabetes incidente, houve associação limítrofe, não-significativa, entre maiores valores de EIMC e glicemia de jejum entre 110 e 125mg/dl em 1998 (?=0,030; IC95%: -0,005 a 0,065). Ambos os níveis de glicemia de jejum alterada em 1998 não se mostraram associados ao CACS ou à variável composta de CACS >= 400 ou eventos cardiovasculares incidentes nos modelos de ajuste completo. Diabetes incidente foi associado a maiores valores de EIMC (em milímetros) (?=0,034; IC95%: 0,015 a 0,053), a CACS >= 400 (Razão de chances=2,84; IC95%: 1,17-6,91) e ao desfecho combinado de CACS >= 400 ou eventos cardiovasculares incidentes (Razão de chances=3,50; IC95%: 1,60-7,65). Conclusões: Glicemia de jejum alterada em 1998, especialmente nos valores mais próximos dos limiares de corte para diabetes, foram associados a maior incidência de diabetes ao longo do seguimento e a maiores valores de EIMC quando da avaliação inicial do ELSA-Brasil. Diabetes incidente entre as avaliações foi associado a maior risco cardiovascular / Introduction: Impaired fasting glucose has been associated with higher risk of incident diabetes, compared to normoglycemic individuals. Although diabetes mellitus is related to atherosclerosis and higher long-term cardiovascular burden, there are conflicting data about the association between impaired fasting glucose and atherosclerotic disease. We aimed (a) to determine diabetes incidence rates in individuals with normal or impaired fasting glucose in 1998 after follow-up of up to 12 years, (b) whether impaired fasting glucose in 1998 and/or incident diabetes were associated with subclinical atherosclerosis in the Brazilian Longitudinal Study of Adult Health (ELSA-Brasil) or the combined variable of non-fatal clinical events or a coronary calcium score >= 400. Methods: We evaluated 1,536 civil servants from the University of São Paulo, who participated in both 1998 (aged 23-63 years) and ELSA-Brasil baseline (2008-2010) assessments and had complete data. We presented crude and adjusted diabetes incident rates for all individuals and then stratified by sex and body mass index (BMI) in 1998. We used crude and adjusted regression models to estimate the association between impaired fasting glucose in 1998 or incident diabetes and coronary intima-media thickness (CIMT), coronary artery calcium score (CACS) and the composite variable of a CACS?400 or incident cardiovascular events (myocardial infarction or revascularization). Results: We found incident diabetes in 177 individuals. Diabetes incidence in our sample was 9.8/1,000 person-years (95% confidence interval [95%CI]:7.7-13.6). Diabetes incidence was higher in men (11.2/1,000 person-years, 95%CI: 8.6-15.0) than women (8.5/1,000 person-years, 95%CI: 5.3 to 15.3). Impaired fasting glucose in 1998 was associated with a higher risk of progression to diabetes during follow-up (hazard ratio [HR]: 3.17; 95%CI: 2.14-4.68 and HR: 7.42; 95%CI: 4.75-11.57 for a fasting plasma glucose between 100 to 109mg/dl and 110 to 125 mg/dl, respectively). Fasting plasma glucose levels between 110 to 125 mg/dl in 1998 were associated with higher CIMT (beta=+0.028; 95%CI: 0.003 to 0.053) in ELSA-Brasil baseline. Excluding those with incident diabetes, there was a non-significant borderline association between higher CIMT (in mm) and fasting plasma glucose 110 to 125mg/dl (beta=0.030; 95%CI: -0.005 to 0.065). Fasting plasma glucose levels in 1998 were not associated with CACS or the composite variable of a CACS ? 400 or incident cardiovascular events in full-adjusted models. Incident diabetes was associated with higher CIMT (in mm) (beta=0.034; 95%CI: 0.015 to 0.053), CACS >= 400 (OR=2.84; 95%CI: 1.17-6.91) and the combined outcome of a CACS >= 400 or incident cardiovascular event (OR=3.50; 95%CI: 1.60-7.65). Conclusions: Elevated fasting plasma glucose in 1998, especially those near diabetes diagnosis limits were associated with higher diabetes incidence during follow-up and higher CIMT in ELSA-Brasil baseline assessment. Incident diabetes between assessments was associated with higher cardiovascular burden Aterosclerose Atherosclerosis Cardiovascular disease Carotid intima-media thickness Complicações do diabetes Diabetes complications Diabetes mellitus Diabetes mellitus Doenças cardiovasculares Epidemiologia Epidemiology Espessura íntima-média carotídea Fatores de risco Glicemia Glucose intolerance Glycemia Hiperglicemia Hyperglycemia Infarto do miocárdio Intolerância à glicose Myocardial infarct Pre-diabetes Pré-diabetes Risk factors
34	Restrição no consumo de sódio durante a gestação é responsável pelo baixo peso ao nascimento e pela resistência à insulina da prole na idade adulta: estudo do mecanismo epigenético por metilação do DNA / Sodium intake restriction during pregnancy is responsible for low birth weight and the insulin resistance of offspring in adulthood: a study of epigenetic mechanism by DNA methylation Siqueira, Flavia Ramos de 14 May 2014 (has links) Sabe-se que algumas alterações nutricionais maternas durante o período perinatal estão associadas com doenças metabólicas na vida adulta das proles, tais como diabetes melito tipo 2, resistência à insulina, obesidade e hipertensão arterial. O período da gestação em que estas alterações nutricionais influenciam a prole na idade adulta ainda não está elucidado. Modificações epigenéticas têm sido propostas como mecanismos responsáveis por estas desordens metabólicas. Ratas Wistar de doze semanas de idade foram alimentadas com dieta com conteúdo baixo (HO - 0,15% NaCl) ou normal (NR - 1,3% NaCl) de sódio desde o primeiro dia de gestação até o nascimento da prole ou HO durante a primeira (HO10) ou segunda (HO20) metade da gestação. O peso corpóreo e a ingestão de água e ração foram avaliados semanalmente durante a gestação. Teste de tolerância à insulina (ITT) e à glicose (GTT) e HOMA-IR foram realizados nas proles adultas. Expressão gênica por qRT-PCR e metilação do DNA na região promotora dos genes foram mapeadas utilizando tratamento com bissulfito de sódio e avaliadas por pirosequenciamento. O ganho de peso materno foi menor no HO e HO20 na terceira semana de gestação em comparação com NR e HO10. O peso ao nascimento da prole foi menor em machos e fêmeas dos grupos HO e HO20 em relação ao NR e HO10. O HOMA-IR foi maior nos machos com 12 semanas de idade do grupo HO em comparação com NR e com 20 semanas de idade do grupo HO10 em comparação com NR e HO20. Nas fêmeas com 12 semanas de idade o HOMA-IR foi maior no HO10 comparado com HO. Os níveis de insulina no soro foram maiores tanto nos machos com 20 semanas de idade do grupo HO10 comparado com NR quanto nas fêmeas com 12 semanas de idade do grupo HO10 comparado com HO. A área sob a curva do GTT indicou intolerância à glicose nos machos do grupo HO. A porcentagem de metilação das ilhas CpG no promotor dos genes de Igf1, Igf1r, Ins1, Ins2 e Insr no fígado de machos e fêmeas neonatais e no fígado, tecido adiposo branco e músculo em machos com 20 semanas de idade foi influenciada pela baixa ingestão de sal durante a gestação. Nenhuma destas alterações foi identificada nas fêmeas com 20 semanas de idade. Em conclusão, a baixa ingestão de sal na segunda metade da gestação é responsável pelo baixo peso ao nascimento em ambos os sexos. A intolerância à glicose observada na prole adulta ocorreu somente se a dieta hipossódica é dada durante a gestação inteira. Por outro lado, a resistência à insulina em resposta ao consumo de dieta hipossódica durante a gestação está relacionada com o momento em que ocorre este insulto e com o envelhecimento da prole. Também foi observado que alterações na metilação do promotor do gene Igf1 está correlacionado com o baixo peso ao nascimento em resposta a ingestão de dieta hipossódica durante a gestação / It is known that some maternal nutritional alterations during pregnancy are associated with metabolic disorders in adult offspring, such as insulin resistance, type 2 diabetes mellitus, obesity and arterial hypertension. The period of pregnancy in which these nutritional alterations influence adult offspring remains uncertain. Epigenetic changes are proposed to underlie these metabolic disorders. Twelve-week-old female Wistar rats were fed a low-salt (LS - 0.15% NaCl) or normal-salt (NS - 1.3% NaCl) diet since the first day of gestation until delivery or LS during the first (LS10) or second (LS20) half of gestation. Body weight, food and water intake were weekly evaluated during gestation. Blood glucose, insulin (ITT) and glucose (GTT) tolerance tests, HOMA-IR were performed in adult offspring. Gene expression and DNA methylation were mapped using bisulfite treatment evaluated by pyrosequencing in the male and female neonates and adult offspring. Weight gain was lower in LS and LS20 dams than in NS and LS10 dams in the third week of pregnancy. Birth weights were lower in male and female LS20 and LS rats compared with NS and LS10 neonates. HOMA-IR was higher in 12-week-old LS males compared with NS and in 20-week-old male LS10 rats compared with NS and LS20 rats. In 12-week-old LS10 females, HOMA-IR was higher than in LS. Serum insulin levels were higher in 20 week-old LS10 male compared with NS rats and in 12-week-old LS10 female compared to LS rats. The area under the curve of GTT indicated glucose intolerance in 12- and 20-week-old LS male. Methylation of CpG islands of the Insr, Igf1, Igf1r, Ins1 and Ins2 genes in liver in neonates male and female offspring and liver, white adipose tissue and muscle in 20-week-old male offspring were influenced by low-salt intake during pregnancy. None of these alterations was identified in 20-week-old females. In conclusion, low-salt diet consumption in the second half of pregnancy can result in low birth weights in the males and females offspring. Glucose intolerance observed in adult offspring occurred only if low salt intake was given throughout pregnancy. However, insulin resistance in response to low salt intake during pregnancy is related to the time at which this insult occurs and to the age of the offspring. Alterations in the DNA methylation of Igf1 were observed to be correlated with low birth weight in response to low salt feeding during pregnancy Baixo peso ao nascer CpG Islands Dieta hipossódica DNA methylation Epigênese genética Epigeneses genetic Expressão gênica Fetal programming Gene expression Glucose intolerance Ilhas de CpG Insulin resistance Insulin-like growth factor 1 Intolerância à glicose Low birth weight Low sodium diet Metilação do DNA Programação fetal Ratos Wistar Rats Wistar Resistência à insulina
35	The role of alpha oxidation in lipid metabolism Jenkins, Benjamin John January 2018 (has links) Recent findings have shown an inverse association between the circulating levels of pentadecanoic acid (C15:0) and heptadecanoic acid (C17:0) with the risk of pathological development in type 2 diabetes, cardio vascular disease and neurological disorders. From previously published research, it has been said that both these odd chain fatty acids are biomarkers of their dietary intake and are significantly correlated to dietary ruminant fat intake. However, there are profound studies that show the contrary where they do not display this biomarker correlation. Additionally, several astute studies have suggested or shown odd chain fatty acid endogenous biosynthesis, most often suggested via alpha oxidation; the cleavage of a single carbon unit from a fatty acid chain within the peroxisomes. To better understand the correlations and interactions between these two fatty acids with pathological development, the origin of these odd chain fatty acids needed to be determined, along with confirming their association with the disease aetiology. To minimise animal & human experimentation we made use of existing sample sets made available through institutional collaborations, which produced both animal and human interventional study samples suitable for odd chain fatty acid investigations. These sample collaborations allowed us to comprehensively investigate all plausible contributory sources of these odd chain fatty acids; including from the intestinal microbiota, from dietary contributions, and derived from novel endogenous biosynthesis. The investigations included two intestinal germ-free studies, two ruminant fat diet studies, two dietary fat studies and an ethanol intake study. Endogenous biosynthesis was assessed through: a stearic acid infusion, phytol supplementation, and an Hacl1 knockout mouse model. A human dietary intervention study was used to translate the results. Finally, a study comparing circulating baseline C15:0 and C17:0 levels with the development of glucose intolerance. We found that the circulating C15:0 and C17:0 levels were not significantly influenced by the presence or absence of intestinal microbiota. The circulating C15:0 levels were significantly and linearly increased when the C15:0 dietary composition increased; however, there was no significant correlation in the circulating C17:0 levels with intake. Circulating levels of C15:0 were affected by the dietary composition and factors affecting the dietary intake, e.g. total fat intake and ethanol, whereas circulating C17:0 levels were found to be independent of these variables. In our studies, the circulating C15:0 levels were not significantly affected by any expected variations in alpha oxidation caused by pathway substrate inhibition or gene knockout. However, C17:0 was significantly related, demonstrating it is substantially endogenously biosynthesised. Furthermore, we found that the circulating C15:0 levels, when independent of any dietary variations, did not correlate with the progression of glucose intolerance when induced, but the circulating C17:0 levels did significantly relate and linearly correlated with the development of glucose intolerance. To summarise, the circulating C15:0 and C17:0 levels were independently derived; the C15:0 levels substantially correlated with its dietary intake, whilst the C17:0 levels proved to be separately derived from its endogenous biosynthesis via alpha oxidation of stearic acid. C15:0 was found to be minimally endogenously biosynthesised via a single cycle of beta oxidation of C17:0 in the peroxisomes, however, this did not significantly contribute to the circulating levels of C15:0. Additionally, only the baseline levels of C17:0 significantly correlated with the development of glucose intolerance. These findings highlight the considerable differences between both of these odd chain fatty acids that were once thought to be homogeneous and similarly derived. On the contrary, they display profound dietary, metabolic, and pathological differences.
36	Glicemia de jejum, diabetes incidente, aterosclerose subclínica e eventos cardiovasculares não-fatais numa amostra de adultos aparentemente saudáveis reavaliados após 12 anos / Fasting plasma glucose, incident diabetes, subclinical atherosclerosis and non-fatal cardiovascular events in an apparently healthy adult sample reevaluated after a 12 years interval Debora Sitnik 01 November 2016 (has links) Introdução: Glicemia de jejum alterada tem sido associada a maior risco de desenvolver diabetes, comparando a indivíduos normoglicêmicos. Apesar de diabetes ser relacionado a aterosclerose e a piores desfechos cardiovasculares, os dados de literatura relacionando glicemia de jejum alterada à doença aterosclerótica são conflitantes. Os objetivos deste trabalho foram determinar (a) a incidência de diabetes em indivíduos com glicemia de jejum normal ou alterada em 1998 após um seguimento de até 12 anos; (b) se a glicemia de jejum alterada em 1998 e/ou diabetes incidente estiveram associados com aterosclerose subclínica no Estudo Longitudinal da Saúde do Adulto (ELSA-Brasil) ou à variável combinada de eventos clínicos não-fatais e escore de cálcio coronariano maior ou igual a 400. Métodos: Avaliamos 1.536 trabalhadores da Universidade de São Paulo, que participaram de um programa de avaliação em 1998 (idade 23-63 anos) e da linha de base do ELSA-Brasil (2008-2010). Apresentamos as taxas de incidência de diabetes brutas e ajustadas para todos os indivíduos e também estratificados por gênero e por índice de massa corpórea (IMC) em 1998. Utilizamos modelos de regressão brutos e ajustados para estimar a associação entre glicemia de jejum alterada em 1998 ou diabetes incidente com a espessura de íntima-média de carótidas (EIMC), escore de cálcio coronariano (CACS, do inglês Coronary Artery Calcium Score) e a variável composta CACS >= 400 ou eventos cardiovasculares incidentes (infarto do miocárdio ou revascularização). Resultados: Encontramos diabetes incidente em 177 indivíduos. A incidência de diabetes em nossa amostra foi de 9,8/1.000 pessoas-ano (Intervalo de confiança de 95% [IC95%]: 7,7-13,6). A incidência foi mais elevada entre os homens (11,2/1.000 pessoas-ano, IC95%: 8,6-15,0) do que entre as mulheres (8,5/1.000 pessoas-ano, IC95%: 5,3-15,3). Glicemia de jejum alterada em 1998 mostrou associação com maior risco de progressão para diabetes ao longo do seguimento (hazard ratio [HR]: 3,17; IC95%: 2,14-4,68) e HR: 7,42; IC95%: 4,75-11,57 para glicemias de jejum entre 100 e 109mg/dl e entre 110 e 125mg/dl, respectivamente). Glicemias entre 110 e 125mg/dl em 1998 foram associadas a maiores valores de EIMC (beta=+0,028; IC95%: 0,003 a 0,053) na linha de base do ELSA-Brasil. Ao excluir da análise aqueles com diabetes incidente, houve associação limítrofe, não-significativa, entre maiores valores de EIMC e glicemia de jejum entre 110 e 125mg/dl em 1998 (?=0,030; IC95%: -0,005 a 0,065). Ambos os níveis de glicemia de jejum alterada em 1998 não se mostraram associados ao CACS ou à variável composta de CACS >= 400 ou eventos cardiovasculares incidentes nos modelos de ajuste completo. Diabetes incidente foi associado a maiores valores de EIMC (em milímetros) (?=0,034; IC95%: 0,015 a 0,053), a CACS >= 400 (Razão de chances=2,84; IC95%: 1,17-6,91) e ao desfecho combinado de CACS >= 400 ou eventos cardiovasculares incidentes (Razão de chances=3,50; IC95%: 1,60-7,65). Conclusões: Glicemia de jejum alterada em 1998, especialmente nos valores mais próximos dos limiares de corte para diabetes, foram associados a maior incidência de diabetes ao longo do seguimento e a maiores valores de EIMC quando da avaliação inicial do ELSA-Brasil. Diabetes incidente entre as avaliações foi associado a maior risco cardiovascular / Introduction: Impaired fasting glucose has been associated with higher risk of incident diabetes, compared to normoglycemic individuals. Although diabetes mellitus is related to atherosclerosis and higher long-term cardiovascular burden, there are conflicting data about the association between impaired fasting glucose and atherosclerotic disease. We aimed (a) to determine diabetes incidence rates in individuals with normal or impaired fasting glucose in 1998 after follow-up of up to 12 years, (b) whether impaired fasting glucose in 1998 and/or incident diabetes were associated with subclinical atherosclerosis in the Brazilian Longitudinal Study of Adult Health (ELSA-Brasil) or the combined variable of non-fatal clinical events or a coronary calcium score >= 400. Methods: We evaluated 1,536 civil servants from the University of São Paulo, who participated in both 1998 (aged 23-63 years) and ELSA-Brasil baseline (2008-2010) assessments and had complete data. We presented crude and adjusted diabetes incident rates for all individuals and then stratified by sex and body mass index (BMI) in 1998. We used crude and adjusted regression models to estimate the association between impaired fasting glucose in 1998 or incident diabetes and coronary intima-media thickness (CIMT), coronary artery calcium score (CACS) and the composite variable of a CACS?400 or incident cardiovascular events (myocardial infarction or revascularization). Results: We found incident diabetes in 177 individuals. Diabetes incidence in our sample was 9.8/1,000 person-years (95% confidence interval [95%CI]:7.7-13.6). Diabetes incidence was higher in men (11.2/1,000 person-years, 95%CI: 8.6-15.0) than women (8.5/1,000 person-years, 95%CI: 5.3 to 15.3). Impaired fasting glucose in 1998 was associated with a higher risk of progression to diabetes during follow-up (hazard ratio [HR]: 3.17; 95%CI: 2.14-4.68 and HR: 7.42; 95%CI: 4.75-11.57 for a fasting plasma glucose between 100 to 109mg/dl and 110 to 125 mg/dl, respectively). Fasting plasma glucose levels between 110 to 125 mg/dl in 1998 were associated with higher CIMT (beta=+0.028; 95%CI: 0.003 to 0.053) in ELSA-Brasil baseline. Excluding those with incident diabetes, there was a non-significant borderline association between higher CIMT (in mm) and fasting plasma glucose 110 to 125mg/dl (beta=0.030; 95%CI: -0.005 to 0.065). Fasting plasma glucose levels in 1998 were not associated with CACS or the composite variable of a CACS ? 400 or incident cardiovascular events in full-adjusted models. Incident diabetes was associated with higher CIMT (in mm) (beta=0.034; 95%CI: 0.015 to 0.053), CACS >= 400 (OR=2.84; 95%CI: 1.17-6.91) and the combined outcome of a CACS >= 400 or incident cardiovascular event (OR=3.50; 95%CI: 1.60-7.65). Conclusions: Elevated fasting plasma glucose in 1998, especially those near diabetes diagnosis limits were associated with higher diabetes incidence during follow-up and higher CIMT in ELSA-Brasil baseline assessment. Incident diabetes between assessments was associated with higher cardiovascular burden Aterosclerose Complicações do diabetes Diabetes mellitus Doenças cardiovasculares Epidemiologia Espessura íntima-média carotídea Fatores de risco Glicemia Hiperglicemia Infarto do miocárdio Intolerância à glicose Pré-diabetes Atherosclerosis Cardiovascular disease Carotid intima-media thickness Diabetes complications Diabetes mellitus Epidemiology Glucose intolerance Glycemia Hyperglycemia Myocardial infarct Pre-diabetes Risk factors
37	Restrição no consumo de sódio durante a gestação é responsável pelo baixo peso ao nascimento e pela resistência à insulina da prole na idade adulta: estudo do mecanismo epigenético por metilação do DNA / Sodium intake restriction during pregnancy is responsible for low birth weight and the insulin resistance of offspring in adulthood: a study of epigenetic mechanism by DNA methylation Flavia Ramos de Siqueira 14 May 2014 (has links) Sabe-se que algumas alterações nutricionais maternas durante o período perinatal estão associadas com doenças metabólicas na vida adulta das proles, tais como diabetes melito tipo 2, resistência à insulina, obesidade e hipertensão arterial. O período da gestação em que estas alterações nutricionais influenciam a prole na idade adulta ainda não está elucidado. Modificações epigenéticas têm sido propostas como mecanismos responsáveis por estas desordens metabólicas. Ratas Wistar de doze semanas de idade foram alimentadas com dieta com conteúdo baixo (HO - 0,15% NaCl) ou normal (NR - 1,3% NaCl) de sódio desde o primeiro dia de gestação até o nascimento da prole ou HO durante a primeira (HO10) ou segunda (HO20) metade da gestação. O peso corpóreo e a ingestão de água e ração foram avaliados semanalmente durante a gestação. Teste de tolerância à insulina (ITT) e à glicose (GTT) e HOMA-IR foram realizados nas proles adultas. Expressão gênica por qRT-PCR e metilação do DNA na região promotora dos genes foram mapeadas utilizando tratamento com bissulfito de sódio e avaliadas por pirosequenciamento. O ganho de peso materno foi menor no HO e HO20 na terceira semana de gestação em comparação com NR e HO10. O peso ao nascimento da prole foi menor em machos e fêmeas dos grupos HO e HO20 em relação ao NR e HO10. O HOMA-IR foi maior nos machos com 12 semanas de idade do grupo HO em comparação com NR e com 20 semanas de idade do grupo HO10 em comparação com NR e HO20. Nas fêmeas com 12 semanas de idade o HOMA-IR foi maior no HO10 comparado com HO. Os níveis de insulina no soro foram maiores tanto nos machos com 20 semanas de idade do grupo HO10 comparado com NR quanto nas fêmeas com 12 semanas de idade do grupo HO10 comparado com HO. A área sob a curva do GTT indicou intolerância à glicose nos machos do grupo HO. A porcentagem de metilação das ilhas CpG no promotor dos genes de Igf1, Igf1r, Ins1, Ins2 e Insr no fígado de machos e fêmeas neonatais e no fígado, tecido adiposo branco e músculo em machos com 20 semanas de idade foi influenciada pela baixa ingestão de sal durante a gestação. Nenhuma destas alterações foi identificada nas fêmeas com 20 semanas de idade. Em conclusão, a baixa ingestão de sal na segunda metade da gestação é responsável pelo baixo peso ao nascimento em ambos os sexos. A intolerância à glicose observada na prole adulta ocorreu somente se a dieta hipossódica é dada durante a gestação inteira. Por outro lado, a resistência à insulina em resposta ao consumo de dieta hipossódica durante a gestação está relacionada com o momento em que ocorre este insulto e com o envelhecimento da prole. Também foi observado que alterações na metilação do promotor do gene Igf1 está correlacionado com o baixo peso ao nascimento em resposta a ingestão de dieta hipossódica durante a gestação / It is known that some maternal nutritional alterations during pregnancy are associated with metabolic disorders in adult offspring, such as insulin resistance, type 2 diabetes mellitus, obesity and arterial hypertension. The period of pregnancy in which these nutritional alterations influence adult offspring remains uncertain. Epigenetic changes are proposed to underlie these metabolic disorders. Twelve-week-old female Wistar rats were fed a low-salt (LS - 0.15% NaCl) or normal-salt (NS - 1.3% NaCl) diet since the first day of gestation until delivery or LS during the first (LS10) or second (LS20) half of gestation. Body weight, food and water intake were weekly evaluated during gestation. Blood glucose, insulin (ITT) and glucose (GTT) tolerance tests, HOMA-IR were performed in adult offspring. Gene expression and DNA methylation were mapped using bisulfite treatment evaluated by pyrosequencing in the male and female neonates and adult offspring. Weight gain was lower in LS and LS20 dams than in NS and LS10 dams in the third week of pregnancy. Birth weights were lower in male and female LS20 and LS rats compared with NS and LS10 neonates. HOMA-IR was higher in 12-week-old LS males compared with NS and in 20-week-old male LS10 rats compared with NS and LS20 rats. In 12-week-old LS10 females, HOMA-IR was higher than in LS. Serum insulin levels were higher in 20 week-old LS10 male compared with NS rats and in 12-week-old LS10 female compared to LS rats. The area under the curve of GTT indicated glucose intolerance in 12- and 20-week-old LS male. Methylation of CpG islands of the Insr, Igf1, Igf1r, Ins1 and Ins2 genes in liver in neonates male and female offspring and liver, white adipose tissue and muscle in 20-week-old male offspring were influenced by low-salt intake during pregnancy. None of these alterations was identified in 20-week-old females. In conclusion, low-salt diet consumption in the second half of pregnancy can result in low birth weights in the males and females offspring. Glucose intolerance observed in adult offspring occurred only if low salt intake was given throughout pregnancy. However, insulin resistance in response to low salt intake during pregnancy is related to the time at which this insult occurs and to the age of the offspring. Alterations in the DNA methylation of Igf1 were observed to be correlated with low birth weight in response to low salt feeding during pregnancy Baixo peso ao nascer Dieta hipossódica Epigênese genética Expressão gênica Ilhas de CpG Intolerância à glicose Metilação do DNA Programação fetal Ratos Wistar Resistência à insulina CpG Islands DNA methylation Epigeneses genetic Fetal programming Gene expression Glucose intolerance Insulin resistance Insulin-like growth factor 1 Low birth weight Low sodium diet Rats Wistar
38	Glucose metabolism in preclinical type 1 diabetes Helminen, O. (Olli) 27 September 2016 (has links) Abstract Type 1 diabetes is considered to be a T cell-mediated autoimmune disease characterized by destruction of the pancreatic beta cells. Its prediction is currently based on diabetes-associated autoantibodies, giving a cumulative risk of 84% during 15 years of follow-up since seroconversion. Prediction of the timing of clinical onset has remained challenging, however. This thesis examines glucose metabolism in autoantibody-positive children with a high risk of developing type 1 diabetes. Out of a total of 14,876 children with an increased genetic risk followed up from birth in the Finnish DIPP study, 567 developed ≥2 autoantibodies during the follow-up and 255 of these (45%) were diagnosed with type 1 diabetes until the end of December 2011. The glucose parameters measured were HbA1c, OGTT and random plasma glucose with 3 to 12 months interval. Seven-day continuous glucose monitoring (CGM) was performed on an age and sex-matched cohort. We showed that rising HbA1c, impaired glucose tolerance in OGTT, random plasma glucose values of ≥7.8mmol/l and potentially CGM can predict type 1 diabetes with a median time to diagnosis of approximately one year. Our results suggest that especially HbA1c and random plasma glucose are cost-effective and improve the prediction of diabetes. These markers may be useful for monitoring the response to treatment in prevention studies. / Tiivistelmä Tyypin 1 diabetesta pidetään T-soluvälitteisenä autoimmuunitautina, joka johtaa haiman beetasolujen tuhoutumiseen. Tyypin 1 diabeteksen ennustaminen perustuu tällä hetkellä diabetekseen assosioituviin vasta-aineisiin, jotka antavat 84% kumulatiivisen riskin 15 vuoden seurannassa. Taudin puhkeamisen ajankohdan ennustaminen on kuitenkin edelleen vaikeaa. Tämä väitöskirja käsittelee glukoosiaineenvaihduntaa vasta-ainepositiivisilla lapsilla, joilla on suurentunut riski sairastua tyypin 1 diabetekseen. Suomalaisessa DIPP-tutkimuksessa vasta-aineiden kehittymistä on seurattu yhteensä 14876 lapselta. Seurannan aikana 567 lasta kehitti ≥2 autovasta-ainetta ja näistä 255 (45%) sairastui tyypin 1 diabetekseen joulukuun loppuun 2011 mennessä. Glukoosiaineenvaihduntaa seurattiin tutkimalla HbA1c, OGTT ja satunnaisia verensokeriarvoja 3-12 kuukauden välein. Ikä ja sukupuolivakioidussa kohortissa tehtiin jatkuvan sokeripitoisuuden seuranta (CGM). Tutkimuksessamme nouseva HbA1c, heikentynyt sokerin sieto OGTT-kokeessa, satunnainen verensokeri ≥7.8 mmol/l ja mahdollisesti CGM ennustavat tyypin 1 diabeteksen puhkeamista. Tulostemme perusteella erityisesti kustannustehokkaat HbA1c ja satunnainen verensokeri parantavat diabeteksen ennustamista. Nämä parametrit saattavat olla hyödyllisiä myös preventiotutkimuksissa hoitovasteen seurannassa. C-peptide autoimmunity continuous glucose monitoring dysglycemia glucose intolerance islet autoantibodies oral glucose tolerance test prediabetes self-monitoring blood glucose type 1 diabetes C-peptidi autovasta-aineet glukoosi-intoleranssi jatkuva sokeripitoisuuden seuranta oraalinen sokerirasituskoe prediabetes sokeriaineenvaihdunnan poikkeavuus tyypin 1 diabetes verensokerin kotimittaus HLA HbA1c

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