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Artykuły w czasopismach na temat "Insulin"
Hansenne, Isabelle Sylvie, Chantal Renard i Vincent Geenen. "Igf2 expression is required for complete tolerance to insulin (128.19)". Journal of Immunology 178, nr 1_Supplement (1.04.2007): S213—S214. http://dx.doi.org/10.4049/jimmunol.178.supp.128.19.
Pełny tekst źródłaShestakova, Marina Vladimirovna, i Irina Vladimirovna Glinkina. "Insulin glargine does not increase the risk of malignancy.Synopsis of the article ?Combined randomised controlled trial experience of malignancies in studies using insulin glargine?byHome P.D. & Lagarenne P. (Diabetologia 2009, vol. 52 (12): 2499-2506)". Diabetes mellitus 13, nr 1 (15.03.2010): 88–90. http://dx.doi.org/10.14341/2072-0351-6022.
Pełny tekst źródłaDąbrowski, Mariusz. "U kogo i dlaczego warto zastosować insulinę dwuanalogową aspart + degludec?" Medycyna Faktów 16, nr 2(59) (30.06.2023): 227–33. http://dx.doi.org/10.24292/01.mf.0223.15.
Pełny tekst źródłaModi, K. D., Pradeep V. Gadge, Pradeep Jain, Sudhir Pawar, Ruchi D. Shah, Shahu A. Ingole i Rishi Jain. "Clinical challenges with excipients in insulin formulations and role of concentrated insulin". International Journal of Basic & Clinical Pharmacology 8, nr 4 (23.03.2019): 821. http://dx.doi.org/10.18203/2319-2003.ijbcp20191125.
Pełny tekst źródłaRay, Sumit. "Insulin infusion protocol (Human insulin®/Insugen®)". Current Medicine Research and Practice 4, nr 4 (lipiec 2014): 186–87. http://dx.doi.org/10.1016/j.cmrp.2014.08.007.
Pełny tekst źródłaKucera, Michelle L., i John P. Graham. "Insulin Lispro, a New Insulin Analog". Pharmacotherapy: The Journal of Human Pharmacology and Drug Therapy 18, nr 3 (6.05.1998): 526–38. http://dx.doi.org/10.1002/j.1875-9114.1998.tb03116.x.
Pełny tekst źródłaZHANG, Zhou. "Protein engineering of insulin: Two novel fast-acting insulins [B16Ala]insulin and [B26Ala]insulin". Science in China Series C 46, nr 5 (2003): 474. http://dx.doi.org/10.1360/01yc0295.
Pełny tekst źródłaHarned, Leighton Kahle, i Edward Chin. "PSUN278 Factitious hypoglycemia, diagnostic delay due to insulin assay failure to detect insulin analogues." Journal of the Endocrine Society 6, Supplement_1 (1.11.2022): A403. http://dx.doi.org/10.1210/jendso/bvac150.838.
Pełny tekst źródłaGargiulo, P., U. Di Mario, O. Zuccarini, F. Troili, C. Tiberti, U. Nicolini, A. Pachi, G. Gerlini i F. Fallucca. "Treatment of diabetic pregnant women with monocomponent insulins". Acta Endocrinologica 113, nr 3_Suppl (sierpień 1986): S60—S65. http://dx.doi.org/10.1530/acta.0.111s0060.
Pełny tekst źródłaMbanya, Jean Claude, Juergen Sandow, Wolfgang Landgraf i David R. Owens. "Recombinant Human Insulin in Global Diabetes Management – Focus on Clinical Efficacy". European Endocrinology 13, nr 01 (2017): 21. http://dx.doi.org/10.17925/ee.2017.13.01.21.
Pełny tekst źródłaRozprawy doktorskie na temat "Insulin"
Guarilha, Alessandra Lia Gasparetti. "Transdução do sinal da insulina em animais expostos ao frio : o papel do cross-talk entre o receptor 'beta' 3 - adrenergico e o receptor de insulina em tecido adiposo marrom". [s.n.], 2004. http://repositorio.unicamp.br/jspui/handle/REPOSIP/310365.
Pełny tekst źródłaTese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas
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Resumo: A exposição de animais homeotérmicos ao mo é utilizada como um método reprodutível para se obter um modelo animal de hipoinsulinemiaacompanhada por elevada mobilização periférica de glicose. No presente estudo, avaliaram-se as etapas iniciais e intermediárias da via de sinalização da insulina em tecidos periféricos de ratos expostos ao mo. Avaliou-se ainda, a comunicação intracelular entre o receptor (33-adrenérgicoe as vias de sinalização da insulina em tecido adiposo marrom de ratos expostos ao mo e tratados, ou não, com compostos agonista ou antagonista (33-adrenérgicos.A exposição de ratos ao mo promoveu a redução da secreção de insulina, acompanhada de um elevado clearance de glicose e maior captação de glicose por tecido muscular esquelético, adiposo branco e adiposo marrom. Tais fenômenos foram acompanhados por inibição da ativação da maior parte dos componentes da via de sinalização da insulina em tecido muscular esquelético e adiposo branco; por estimulação da maior parte dos componentes da via de sinalização da insulina em tecido adiposo marrom; e por efeitos variados (estímulo, inibição e não-modulação) de componentes da via de sinalização da insulina em figado. Por fim, este estudo demonstrou que a exposição ao mo ativa a sinalização (33-adrenérgicaem tecido adiposo marrom. Tal ativação leva à modulação da atividade de vários componentes da via de sinalização da insulina neste tecido. Entretanto, fatores independentes da sinalização (33-adrenérgica parecem contribuir para a complexa regulação do sinal da insulina obseIVada em tecido adiposo marrom de ratos expostos ao mo. Em conclusão, o presente estudo revelou alguns dos intrincados mecanismos pelos quais a exposição ao mo controla a atividade da insulina em animais homeotérmicos, podendo favorecer a identificação de potenciais alvos para a ação terapêutica em doenças onde a resistência à insulina desempenha papel central
Abstract: Cold exposure provides a reproducible model of improved glucose turnover accompanied by reduced blood levels of insulin. In the present study, the initial and intermediate steps of the insulin-signaling pathway in peripheral tissues of rats exposed to cold environment were evaluated. Also, the intracellular connection between insulin and ~3-adrenergic signaling in brown adipose tissue of cold exposed rats treated, or not, with ~3-adrenergic agonist or antagonist compounds were evaluated. During cold exposure, insulin secretion was significantly impaired, while whole body glucose clearance rates were significantly improved. This was accompanied by an increased glucose uptake by skeletal muscle, white adipose tissue and brown adipose tissue. These phenomena were paralleled by an apparent molecular resistance to insulin in skeletal muscle and white adipose tissue; by improved molecular response to insulin in brown adipose tissue; and by ambiguous effects (stimulation, inhibition and not modulation) of regulation of the insulin-signaling pathway in liver. Finally, cold exposure activated the ~3-adrenergic signaling in brown adipose tissue. It leads to modulation of activity of several components of the insulin signal transduction pathway in this tissue. However, ~3-adrenergic receptor independent mechanisms seem to contribute to the complex regulation of the insulin signaling observed in brown adipose tissue of rats exposed to cold. In conclusion, the present study revealed some of the complex mechanisms that participate in the cold-exposure-induced control of the insulin action in homeothermic animals. These results may favour the identification of novel potential targets for therapeutics in diabetes and related disorders
Doutorado
Medicina Experimental
Doutor em Fisiopatologia Medica
Aili, Fagerholm Siri. "Insulin signaling in primary adipocytes in insulin sensitive and insulin resistant states". Doctoral thesis, Linköpings universitet, Avdelningen för cellbiologi, 2013. http://urn.kb.se/resolve?urn=urn:nbn:se:liu:diva-95562.
Pełny tekst źródłaProtzek, André Otavio Peres 1984. "Increased insulin secretion and decreased insulin clearance contributes to the hyperinsulinemia in rats and mice treated with glucocorticoid = Aumento da secreção e redução do clearance de insulina contribuem para a hiperinsulinemia compensatória em ratos e camundongos tratados com glicocorticoide". [s.n.], 2013. http://repositorio.unicamp.br/jspui/handle/REPOSIP/313949.
Pełny tekst źródłaTese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia
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Resumo: Os glicocorticoides (GC) são amplamente utilizados devido aos seus efeitos anti-inflamatórios. Porém, o tratamento com GC pode induzir efeitos deletérios sobre a homeostase glicêmica como a resistência à insulina (RI), intolerância à glicose e, dependendo do tempo e dose, pode levar a instalação do Diabetes mellitus tipo 2 (DM2). Neste sentido, ratos têm sido vastamente utilizados como modelo animal para elucidar as compensações pancreáticas envolvidas na hiperinsulinemia induzida por GC e, poucos estudos enfocando os efeitos do tratamento com GC foram realizados em camundongos. Além disso, não é completamente elucidado se a hiperinsulinemia compensatória induzida pelo tratamento com GC esta associada com alteração do clearance de insulina. Assim, nossos objetivos foram avaliar se: as compensações do pâncreas endócrino em resposta ao tratamento com GC são similares entre camundongos e ratos e, identificar possíveis mecanismos que as expliquem; e se a hiperinsulinemia compensatória induzida pelo tratamento com GC em camundongos e ratos esta associada com alterações do clearance de insulina e a expressão da proteína insuling degrading enzyme (IDE) no fígado. Para isto, camundongos Swiss e ratos Wistar machos foram tratados com o glicocorticoide sintético dexametasona (1 mg/kg p.c.; 5 dias consecutivos). O tratamento com GC induziu RI, hiperinsulinemia e dislipidemia em ambas as espécies, embora mais pronunciado em ratos, que também apresentaram intolerância à glicose e hiperglicemia no jejum. Ambas as espécies tratadas com GC apresentaram incremento da secreção de insulina ex vivo estimulada com glicose, massa e proliferação de células ?, que foram associados com aumento da sinalização da via Ir-?/AKT/mTOR e redução da via AMPK/ACC/AS160 em ilhotas isoladas. O clearance de insulina reduziu em camundongos e ratos tratados com GC, o que foi associado com redução da expressão de IDE no fígado. Desta forma, nossos resultados indicam que camundongos são menos sensíveis aos efeitos deletérios do tratamento com GC sobre a homeostase glicêmica, quando comparado com ratos. Ainda, camundongos e ratos apresentam compensações pancreáticas semelhantes (incremento da função e massa de células ?) em resposta ao tratamento com GC, que foi associado com aumento da sinalização da via canônica de insulina e redução da via não canônica em ilhotas isoladas. Além disso, a redução do clearance de insulina foi, ao menos em parte, devido a redução da expressão de IDE no fígado, o que contribuiu para a hiperinsulinemia compensatória em ambas as espécies tratadas com GC. Em conclusão, estes resultados corroboram a hipótese de que fármacos que inibam a expressão ou atividade da IDE no fígado podem ser uma intervenção anti-diabetogênica que auxilie na manutenção da homeostase glicêmica sem sobrecarregar as células ?
Abstract: Glucocorticoids (GCs) are widely used as anti-inflammatory agent, but they may induce adverse metabolic effects such as insulin resistance (IR), glucose intolerance, and occasionally, diabetes mellitus type 2. Healthy rats have been used as animal models to elucidate the islet compensatory mechanisms involved in these metabolic disturbances, and only a few studies, which have focused on the in vivo effects of GCs, have been conducted in mice models. Yet, whether the reduced insulin clearance also contributes to the compensatory hyperinsulinemia in GC-treated rodents is not fully understood. Here, we aimed to elucidate whether mice and rats share the pancreatic compensations that result in response to dexamethasone (DEX) treatment and also to identify the possible mechanisms that can explain its effects. Yet, we investigated whether the hyperinsulinemia induced by GC treatment in mice and rats is associated with altered hepatic insulin degrading enzyme (IDE) expression and insulin clearance. For this, male Swiss mice and Wistar rats were treated with the synthetic GC dexamethasone (1 mg/kg b.w.; 5 days). DEX treatment induced IR, hyperinsulinemia and dyslipidemia in both species (there was a higher magnitude in rats), but treatment had a greater effect in rats that had glucose intolerance and increased basal blood glucose compared to the control group. Ex vivo insulin secretion at different glucose concentrations was higher in both groups of DEX-treated rodents compared to their controls. Mice and rats showed a significant increase in ?-cell mass due to increased ?-cell proliferation, which was associated with upregulation of the Ir-?/AKT/mTOR and downregulation of AMPK/ACC/AS160 signaling. Insulin clearance reduced in GC-treated mice and rats, which were associated with reduced hepatic IDE expression. Thus, mice are less vulnerable than rats to the deleterious effect of GCs on glucose homeostasis. In addition, rats and mice share common islet compensations (increased ?-cell function and mass) in response to GC treatment, which were associated with increased canonical and decreased non-canonical insulin signaling. Farther, the reduced insulin clearance in GC-treated rodents was, at least in part, due to reduced hepatic IDE expression, which contributed to the compensatory hyperinsulinemia. These findings corroborate the idea that pharmacological interventions that inhibit hepatic IDE may be an alternative anti-diabetic agent that helps to maintain glucose homeostasis due to hyperinsulinemia instead of hypoglycemic agent, which increase the overload in the ?-cells and may lead to ?-cell failure and DM2
Doutorado
Fisiologia
Doutor em Biologia Funcional e Molecular
Tavare, J. M. "The insulin receptor and insulin stimulated protein kinase : Their role in insulin action". Thesis, University of Bristol, 1985. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.370675.
Pełny tekst źródłaMoraes, Keila Aziz Chehoud de [UNESP]. "Efeitos decorrentes da ingestão do fluoreto na sensibilidade à insulina e transdução do sinal insulínico". Universidade Estadual Paulista (UNESP), 2006. http://hdl.handle.net/11449/95423.
Pełny tekst źródłaFundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)
Nos últimos anos tem ocorrido uma redução acentuada nos índices de cárie dentária em diversas regiões do planeta, fato que tem se atribuído ao consumo de produtos fluoretados. Entretanto, o flúor, quando ingerido em excesso, causa intoxicação crônica ou aguda, como a fluorose dentária e distúrbios na homeostase da glicose. As crianças se tornam foco de preocupação, principalmente às portadoras de diabetes mellitus (DM), pois geralmente ingerem grandes quantidades de dentifrício fluoretado durante a escovação, ultrapassando a dose preconizada como limite de ingestão diária de flúor de 0,05 a 0,07mg/F/kg de peso corpóreo. Este trabalho, que foi dividido em duas partes, pretende realizar uma breve revisão de literatura sobre os efeitos decorrentes da ingestão de NaF no metabolismo de carboidratos e avaliar os efeitos da ingestão do fluoreto na sensibilidade à insulina e na transdução do sinal insulínico. A primeira parte, baseada em artigos científicos publicados, procura discorrer sobre os efeitos da ingestão de flúor no metabolismo de carboidratos, na tolerância à glicose e no sinal insulínico, e algumas considerações sobre o diabetes mellitus e sobre as possíveis complicações que a ingestão de NaF pode ocasionar às crianças portadoras desta doença. Estes trabalhos demonstraram que o tratamento agudo ou prolongado com altas doses de fluoreto de sódio interfere na homeostase da glicose. Convém salientar que esta alteração é similar à observada em casos de diabetes mellitus. Além do mais, o flúor quando ingerido em excesso, também ocasiona diminuição da secreção de insulina, inibição da glicólise e depleção de glicogênio. Muitas dessas respostas sugerem que o NaF pode promover resistência à insulina. Portanto, a ingestão em excesso de NaF pode prejudicar a saúde, principalmente de crianças portadora de DM.
Over the last few years there has been a significant reduction in the incidence of dental caries in several regions of the world. This has been attributed to the consumption of fluoridated products. However, excess of fluoride intake can cause chronic or acute intoxication, such as dental fluorosis and impaired glucose homeostasis. Concern is focused on children, especially those with diabetes mellitus, because children usually swallow large amounts of fluoridated dentifrice during tooth brushing, in excess of the maximum recommended daily fluoride dose of 0.05 to 0.07 mg/F/kg of body weight. This report, divided into two parts, intends to make a brief literature review about effects of NAF intake on glucose metabolism, and to determine the effects of this intake on insulin sensitivity and insulin signal transduction. The first part, based on published scientific articles, endeavors to describe the effects of NaF intake on glucose metabolism, glucose tolerance and insulin signal, and put forward considerations concerning diabetes mellitus (DM), and the possible complications that NaF intake could cause in children with DM. These reports demonstrated that the acute or chronic treatment with high sodium fluoride dose interferes in glucose homeostasis, resulting in conditions such as hyperglycemia. This alteration is similar to that observed in DM. Furthermore, NaF ingestion in high doses can produce abnormalities in insulin secretion, glycolysis inhibition, and glycogen depletion. Many of these evidences suggest that NaF can induce insulin resistance. Thus, excessive fluoride consumption could worsen health, particularly of diabetic children. Based on that fluoride can interfere in the glucose metabolism, it is important for the second part of this report to determine the acute effect of fluoride on insulin sensitivity and pp185 (IRS-1/IRS-2) phosphorylation in insulin sensitive tissues.
Bertelli, Daniela Faleiros. "Mecanismos moleculares envolvidos no controle da ingestão alimentar e do peso corporal : participação da 5PTASE IV". [s.n.], 2006. http://repositorio.unicamp.br/jspui/handle/REPOSIP/312921.
Pełny tekst źródłaTese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas
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Resumo: A enzima fosfatidilinositol 3-quinase (PI3-kinase) exerce uma importante função na transdução dos sinais anorexigênicos e termogênicos enviados pela insulina e leptina em primeira ordem aos neurônios do núcleo arqueado no hipotálamo. A cascata de sinais intracelulares gerados pela ativação da PI3-kinase depende da atividade coordenada de inositol-fosfatases específicas. Neste trabalho, mostramos que a phosphoinositide-specific inositol polyphosphate 5-phosphatase IV (5ptase IV) está altamente expressa em neurônios do núcleo arqueado e lateral do hipotálamo. Submetido ao tratamento intracerebroventricular (ICV) com insulina, a 5ptase IV sofre fosforilação em tirosina de acordo com um padrão tempo-dependente, a qual segue os mesmos moldes da sinalização da insulina através do seu receptor (IR), seu substrato-2 (IRS2) e da PI3-kinase. Para avaliar a participação da 5ptase IV na ação da insulina no hipotálamo, trabalhamos com um oligonucleotídeo antisense específico para esta enzima. O tratamento dos ratos com este oligonucleotídeo durante quatro dias reduziu a expressão hipotalâmica da 5ptase IV em aproximadamente 80%. Tal fato foi acompanhado pela redução de 70% na sua fosforilação induzida pela insulina, e ainda pelo aumento na quantidade basal dos inositóis fosforilados no hipotálamo. Finalmente, a inibição da expressão da 5ptase IV no hipotálamo pelo oligonucleotídeo antisense, resultou na redução da ingestão média diária de alimentos, na perda de massa corporal e ainda na redução da ingestão alimentar em 12 horas. Desta forma, a 5ptase IV é um potente regulador da sinalização através da PI3kinase no hipotálamo e pode tornar-se um alvo interessante para a terapêutica da obesidade e para as desordens relacionadas
Abstract: The enzyme phosphatidylinositol 3-kinase (PI 3-kinase) exerts an important role in the transduction of the anorexigenic and thermogenic signals delivered by insulin and leptin to first-order neurons of the arcuate nucleus in the hypothalamus. The termination of the intracellular signals generated by the activation of PI 3-kinase depends on the coordinated activity of specific inositol phosphatases. Here, we show that phosphoinositide-specific inositol polyphosphate 5-phosphatase IV (5ptase IV) is highly expressed in neurons of the arcuate and lateral nuclei of the hypothalamus. Upon intracerebroventicular (ICV) treatment with insulin, 5ptase IV undergoes a time-dependent tyrosine phosphorylation, which follows the same patterns of canonical insulin signaling through the insulin receptor, IRS-2, and PI 3-kinase. To evaluate the participation of 5ptase IV in insulin action in hypothalamus, we employed a phosphorthioate modified antisense oligonucleotide specific for this enzyme. The treatment of rats with this oligonucleotide for four days reduced the hypothalamic expression of 5ptase IV by ~80%. This was accompanied by a ~70% reduction of insulin-induced tyrosine phosphorylation of 5ptase IV and by an increase in basal accumulation of phosphorylated inositols in the hypothalamus. Finally, inhibition of hypothalamic 5ptase IV expression by the antisense approach resulted in reduced daily food intake, body weight loss and decreased 12 h spontaneous food intake. Thus, 5ptase IV is a powerful regulator of signaling through PI 3-kinase in hypothalamus and may become an interesting target for therapeutics of obesity and related disorders
Doutorado
Biologia Estrutural, Celular, Molecular e do Desenvolvimento
Doutor em Fisiopatologia Medica
Hagihara, Graziela Neves. "Resposta à angiotensina II em artérias mesentéricas de resistência na obesidade: participação das MAPKs". Universidade de São Paulo, 2012. http://www.teses.usp.br/teses/disponiveis/42/42136/tde-18092012-095317/.
Pełny tekst źródłaAngiotensin II (AngII) can activate mitogen-activated protein kinases (MAPKs) pathways. We investigated the role of obesity and MAPKs in AngII response in monosodium glutamate-induced obese rats (Ob). Endothelium-intact but not endothelium-denuded mesenteric resistance arteries isolated from Ob exhibited a lower response to AngII. The response to nordrenaline and potassium chloride were unaltered. Increased expression of AT2 receptor, nitric oxide synthase (eNOS) and ERK1/2 might be involved in the reduced response since inhibition of AT2R, eNOS and ERK1/2 corrected it. Increased activation of ERK 1/2 in Ob might activate eNOS, generating more NO and vasodilation that contributed to reduce the contraction to AngII. We concluded that, in obesity, the lower response to AngII might be an adaptive mechanism against the increased activation of the renin-angiotensin system. This mechanism involves the participation of the endothelium through a greater release of NO, increased AT2R, eNOS and ERK1/2 expressions.
Pacheco, Calderón Javier, Fernández Paloma Salas i Rigo-Righi Carla Galli. "Vanadium Insulin mimetic activity". Revista de Química, 2012. http://repositorio.pucp.edu.pe/index/handle/123456789/100049.
Pełny tekst źródłaDiabetes mellitus is a serious chronic metabolic disordercharacterized by an increased plasma glucose concentrationand vascular and neurologic complications as well. Diabetesmellitus results from relative or absolute deficiency of insulinsecretion or insulin deficient action. Although there are anumber of oral antidiabetic agents besides insulin or insulinanalogues, none of them is optimal.Vanadium can mimic insulin effects in vitro and in vivoand the possibility of using vanadium compounds asantidiabetic agents is under study. This review will summarizethe insulin mimetic action of vanadium and its possiblemechanisms in comparison with insulin.
Capetini, Vinícius Cooper. "Efeito da suplementação com zinco na evolução da resistência à insulina induzida por dieta hiperlipídica em camundongos". Universidade de São Paulo, 2016. http://www.teses.usp.br/teses/disponiveis/42/42137/tde-10082016-154401/.
Pełny tekst źródłaThe increase in prevalence of type 2 diabetes mellitus (DM2) is intense and implies broad quest for prevention and treatment of disease. Studies have shown the participation of zinc in the synthesis, secretion and signaling pathway of insulin and the glucose control. This study aimed to analyze the mechanism of action of zinc in the control of insulin secretion and glucose control in order to understand whether supplementation with zinc prevents or delays the manifestation of DM2. The project was approved by CEUA-ICB (USP). Male mice C57BL/6 were divided en 4 groups: control diet (NFD); control diet supplemented with ZnCl2 (NFDZ); high fat diet (HFD); and high fat diet supplemented with ZnCl2 (HFDZ). Body weight, feed intake and water and the glucose levels were monitored weekly. Intraperitoneal glucose tolerance test (ipGTT) and insulin (ipITT) were performed at the 14th week of treatment. Completing the 15 weeks of the treatment glycemia, insulinemia and zincemia were analyzed, being applied HOMA-IR and HOMA-β tests. In isolated islets was assessed the static insulin secretion at different glucose concentrations. The uptake and glucose metabolism test was done in the soleus muscle and the content analysis of the AKT and GSK3-β protein was made in the soleus muscle and liver. The data (mean ± SEM) were analyzed by two-way ANOVA with Bonferoni post-test or Student\'s t test (P < 0,05). Zinc supplementation improves glucose dysfunction induced by high fat diet, without nonetheless affecting insulin resistance and insulin secretion by isolated islets.
Gormley, M. J. J. "Aspects of insulin treatment of non-insulin-dependent diabetes". Thesis, Queen's University Belfast, 1985. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.373006.
Pełny tekst źródłaKsiążki na temat "Insulin"
Cuatrecasas, Pedro, i Steven Jacobs, red. Insulin. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5.
Pełny tekst źródłaBrian, Kahn. Insulin. Cambridge: Cambridge Micro Software, 1987.
Znajdź pełny tekst źródłaUnited States. Food and Drug Administration. Office of Women's Health. Insulin. Washington, D.C.]: Dept. of Health and Human Services, FDA, Office of Women's Health, 2010.
Znajdź pełny tekst źródłaPedro, Cuatrecasas, Jacobs Steven 1946- i Avruch J, red. Insulin. Berlin: Springer-Verlag, 1990.
Znajdź pełny tekst źródłaEleazar, Shafrir, i Hansen Barbara C, red. Insulin resistance and insulin resistance syndrome. London: Taylor & Francis, 2002.
Znajdź pełny tekst źródłaZeitler, Philip S., i Kristen J. Nadeau, red. Insulin Resistance. Cham: Springer International Publishing, 2020. http://dx.doi.org/10.1007/978-3-030-25057-7.
Pełny tekst źródłaSrivastava, Ashok K., i Barry I. Posner, red. Insulin Action. Boston, MA: Springer US, 1998. http://dx.doi.org/10.1007/978-1-4615-5647-3.
Pełny tekst źródłaReaven, Gerald M., i Ami Laws, red. Insulin Resistance. Totowa, NJ: Humana Press, 1999. http://dx.doi.org/10.1007/978-1-59259-716-1.
Pełny tekst źródłaStrachan, Mark W. J., i Brian M. Frier. Insulin Therapy. London: Springer London, 2013. http://dx.doi.org/10.1007/978-1-4471-4760-2.
Pełny tekst źródłaZeitler, Philip Scott, i Kristen J. Nadeau, red. Insulin Resistance. Totowa, NJ: Humana Press, 2009. http://dx.doi.org/10.1007/978-1-59745-192-5.
Pełny tekst źródłaCzęści książek na temat "Insulin"
Titchener, Janet. "Insulins and insulin management". W Diabetes Management, 25–37. First edition. | Boca Raton: CRC Press, 2020.: CRC Press, 2020. http://dx.doi.org/10.1201/9780429326196-6.
Pełny tekst źródłaTitchener, Janet. "Insulins and insulin management". W Diabetes Management, 25–37. First edition. | Boca Raton: CRC Press, 2020.: CRC Press, 2020. http://dx.doi.org/10.4324/9780429326196-6.
Pełny tekst źródłaBrandenburg, D. "Insulin Chemistry". W Insulin, 3–22. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_1.
Pełny tekst źródłaHollenberg, M. D. "Insulin Receptor-Mediated Transmembrane Signalling". W Insulin, 183–207. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_10.
Pełny tekst źródłaRothenberg, P., M. F. White i C. R. Kahn. "The Insulin Receptor Tyrosine Kinase". W Insulin, 209–36. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_11.
Pełny tekst źródłaLevy, J. R., i J. M. Olefsky. "Receptor-Mediated Internalization and Turnover". W Insulin, 237–66. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_12.
Pełny tekst źródłaJacobs, S. "Insulin-like Growth Factor I Receptors". W Insulin, 267–86. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_13.
Pełny tekst źródłaSaltiel, A. R., i P. Cuatrecasas. "Second Messengers of Insulin Action". W Insulin, 289–311. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_14.
Pełny tekst źródłaAvruch, J., H. E. Tornqvist, J. R. Gunsalus, E. J. Yurkow, J. M. Kyriakis i D. J. Price. "Insulin Regulation of Protein Phosphorylation". W Insulin, 313–66. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_15.
Pełny tekst źródłaLarner, J. "Effects of Insulin on Glycogen Metabolism". W Insulin, 367–84. Berlin, Heidelberg: Springer Berlin Heidelberg, 1990. http://dx.doi.org/10.1007/978-3-642-74098-5_16.
Pełny tekst źródłaStreszczenia konferencji na temat "Insulin"
Perez, Daniel L., i Ivo Braganza. "Reimagining the Insulin Pump User Experience". W 2024 IEEE Integrated STEM Education Conference (ISEC), 1. IEEE, 2024. http://dx.doi.org/10.1109/isec61299.2024.10664701.
Pełny tekst źródłaGoodwin, P. "Obesity, Insulin Resistance and Insulin." W Abstracts: Thirty-Second Annual CTRC‐AACR San Antonio Breast Cancer Symposium‐‐ Dec 10‐13, 2009; San Antonio, TX. American Association for Cancer Research, 2009. http://dx.doi.org/10.1158/0008-5472.sabcs-09-ms2-1.
Pełny tekst źródłaLin, J., P. Docherty, A. Le Compte, U. Jamaludin, C. E. Hann, N. N. Razak, J. G. Chase, C. G. Pretty i G. M. Shaw. "Modeled Insulin Sensitivity and Interstitial Insulin Action from a Pilot Study of Dynamic Insulin Sensitivity Tests". W UKACC International Conference on CONTROL 2010. Institution of Engineering and Technology, 2010. http://dx.doi.org/10.1049/ic.2010.0358.
Pełny tekst źródłaJayaraj, Nivethitha, C. Mathew Cherian i S. Ganesh Vaidyanathan. "Intelligent Insulin Infuser". W 2009 Third UKSim European Symposium on Computer Modeling and Simulation. IEEE, 2009. http://dx.doi.org/10.1109/ems.2009.64.
Pełny tekst źródłaVereshchetin, Paul, Marc Breton i Stephen D. Patek. "Mealtime correction insulin advisor for CGM-informed insulin pen therapy". W 2013 American Control Conference (ACC). IEEE, 2013. http://dx.doi.org/10.1109/acc.2013.6580277.
Pełny tekst źródłaCesar, Palerm,. "Physiologic Insulin Delivery with Insulin Feedback: A Control Systems Perspective". W Modeling and Control in Biomedical Systems, redaktor Rees, Stephen, chair Andreassen, Steen i Andreassen, Steen. Elsevier, 2009. http://dx.doi.org/10.3182/20090812-3-dk-2006.00006.
Pełny tekst źródłaBaura, Gail D., David M. Foster i Michael W. Schwartz. "Insulin receptors facilitate insulin transport into the central nervous system". W 1992 14th Annual International Conference of the IEEE Engineering in Medicine and Biology Society. IEEE, 1992. http://dx.doi.org/10.1109/iembs.1992.5761454.
Pełny tekst źródłaBaura, Foster i Schwartz. "Insulin Receptors Facilitate Insulin Transport Into The Central Nervous System". W Proceedings of the Annual International Conference of the IEEE Engineering in Medicine and Biology Society. IEEE, 1992. http://dx.doi.org/10.1109/iembs.1992.592647.
Pełny tekst źródłaNowak-Göttl, U., W. D. Kreuz, M. John, B. Krackhardt, H.-P. Grüttner, H. K. Breddin i F. kollmann. "HAEMOSTASEOLOGICAL CHANGES IN DIABETIC CHILDREN (HUMAN INSULIN VERSUS PORCINE INSULIN". W XIth International Congress on Thrombosis and Haemostasis. Schattauer GmbH, 1987. http://dx.doi.org/10.1055/s-0038-1643099.
Pełny tekst źródłaKlenner, Jacob B., Benjamin A. Van Noorden, Jennifer L. Knopp, Lui R. Holder Pearson, Anna R. Hardy, Sarah L. Vergeer, Geoffrey M. Shaw i J. Chase. "Determining the effects of insulin Detemir on endogenous secretion of insulin". W 2019 41st Annual International Conference of the IEEE Engineering in Medicine & Biology Society (EMBC). IEEE, 2019. http://dx.doi.org/10.1109/embc.2019.8857643.
Pełny tekst źródłaRaporty organizacyjne na temat "Insulin"
Anthony Di Franco, Anthony Di Franco. Open Insulin. Experiment, lipiec 2015. http://dx.doi.org/10.18258/5755.
Pełny tekst źródłaMuti, Paola. Insulin and Breast Cancer Risk. Fort Belvoir, VA: Defense Technical Information Center, czerwiec 2001. http://dx.doi.org/10.21236/ada395852.
Pełny tekst źródłaMuti, Paola. Insulin and Breast Cancer Risk. Fort Belvoir, VA: Defense Technical Information Center, czerwiec 2000. http://dx.doi.org/10.21236/ada383382.
Pełny tekst źródłaSilva, Rodrigo Ribeiro e., Mateus de Miranda Gauza, Julia Opolski Nunes da Silva Opolski i Maria Eduarda Schramm Guisso. Once-Weekly Insulin Icodec vs Once-Daily Insulin Glargine U100 for Type 2 Diabetes: A Meta-analysis of Phase 2 Randomized Controlled Trials. INPLASY - International Platform of Registered Systematic Review and Meta-analysis Protocols, maj 2022. http://dx.doi.org/10.37766/inplasy2022.5.0102.
Pełny tekst źródłaLong, Cong, XUke Han, Yunjiao Yang, Tongyi Li, Qian Zhou i Qiu Chen. Efficacy of Intranasal Insulin in Improving Cognition in Mild Cognitive Impairment or Dementia: A Systematic Review and Meta-analysis. INPLASY - International Platform of Registered Systematic Review and Meta-analysis Protocols, sierpień 2022. http://dx.doi.org/10.37766/inplasy2022.8.0054.
Pełny tekst źródłaZHU, Dongshan. The lifestyle changes after initiating basal insulin in insulin naive patients with type 2 diabetes: Results from the ORBIT study. Science Repository, czerwiec 2019. http://dx.doi.org/10.31487/j.jicoa.2019.02.04.
Pełny tekst źródłaShi, Jinping, Feng L, Liting X, Jing L i Xing L. Meta analysis of efficacy and safety of insulin aspart and biosynthetic human insulin in the treatment of gestational diabetes mellitus. Xi'an International Medical Center Hospital, lipiec 2021. http://dx.doi.org/10.37766/inplasy2021.7.0047.
Pełny tekst źródłaChen, Jiankun, Yingming Gu, Lihong Yin, Minyi He, Na Liu, Yue Lu, Changcai Xie, Jiqiang Li i Yu Chen. Network meta-analysis of curative efficacy of different acupuncture methods on obesity combined with insulin resistance. INPLASY - International Platform of Registered Systematic Review and Meta-analysis Protocols, sierpień 2022. http://dx.doi.org/10.37766/inplasy2022.8.0075.
Pełny tekst źródłaCleveland, Rebecca J., Marilie D. Gammon i Ralph S. Baric. Insulin-Like Growth Factor I Polymorphisms in Breast Cancer. Fort Belvoir, VA: Defense Technical Information Center, wrzesień 2002. http://dx.doi.org/10.21236/ada412654.
Pełny tekst źródłaSmith, Nadine, Michael Pishko, Robert Gabbay i Jacob Werner. Closed-Loop Noninvasive Ultrasound Glucose Sensing and Insulin Delivery. Fort Belvoir, VA: Defense Technical Information Center, wrzesień 2006. http://dx.doi.org/10.21236/ada458974.
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