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Determinacao de elementos em sangue de hamster dourado usando AAN / Determination of elements in blood of golden hamster by NAAAGUIAR, RODRIGO O. de 09 October 2014 (has links)
Made available in DSpace on 2014-10-09T12:26:12Z (GMT). No. of bitstreams: 0 / Made available in DSpace on 2014-10-09T14:10:39Z (GMT). No. of bitstreams: 0 / No presente estudo a técnica de analise por ativação com nêutrons foi utilizada para a determinação simultânea da concentração de elementos, de relevância em clínica, em sangue total de Hamster Dourado. O limite de normalidade obtido para Br, Ca Cl, Mg, Na e S considerando 2 (Dois Desvios Padrão), foi de 0,011 - 0,047 gL-1 (Br); 0,11 - 0,35 gL-1 (Ca); 2,11 - 3,75 gL-1 (Cl); 1,35 - 2,79 gL-1 (K), 0,026 0,090 gL-1 (Mg), 1,03 2,51 gL-1 (Na) e 0,97 2,01 gL-1 (S) . O conhecimento desses limites viabiliza o uso de sangue total em investigações clínicas deste modelo animal. A comparação com as estimativas de normalidade em sangue total em seres humanos (Hamster & humano) permitiu verificar as similaridades ou diferenças fisiológicas, dados importantes em experimentos utilizando este modelo animal. / Dissertacao (Mestrado) / IPEN/D / Instituto de Pesquisas Energeticas e Nucleares - IPEN-CNEN/SP
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Studies of cell population kinetics in the hamster cheek pouch, with reference to the difference in growth between normal and malignant cellsReiskin, Allan B. January 1966 (has links)
No description available.
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Muscle spindle morphology in the tenuissimus muscle of the golden syrian hamsterPatten, Robert Michael January 1990 (has links)
The tenuissimus is a long, thin hindlimb skeletal muscle which in hamsters contains about 200 extrafusal muscle fibers. Embedded in this richly innervated muscle is a continuous array of 16-20 closely packed muscle spindles suggesting that it may play a role in hindlimb proprioception. This high spindle density also makes the muscle ideal for the isolation and harvesting of these sensory receptors. In this correlative light and electron microscopic study, freshly frozen specimens were first prepared for serial microscopic analysis. Camera lucida reconstruction of spindle distribution showed a close proximity to the main artery and nerve in the central core of the muscle. Oxidative enzyme and myosin ATPase staining profiles were examined in both the intrafusal and extrafusal fiber populations. Type I and type II extrafusal fibers were present in even numbers and were distributed evenly throughout muscle cross-sections. Enzyme staining varied along the lengths of the three intrafusal fiber types. The fine structure of spindles was examined using transmission (TEM), conventional scanning (SEM), and high resolution scanning electron microscopy (HRSEM). For conventional SEM, isolated spindles were first fixed in 2.5% buffered glutaraldehyde, followed by 1% osmication, and mechanical disruption of the outer capsule under the dissecting microscope. Preparation for HRSEM included aldehyde/osmium fixation and freeze-cleavage of entire tenuissimus muscles in liquid N₂. Selective extraction of the cytosol with 0.1% OsO4
permitted the visualization of numerous intracellular structures. In these specimens, the capsular sleeve showed a multilayered pattern of vesicle-laden cells with variant surface topography in certain locations. Punctate sensory nerve endings adhered intimately to the surfaces of underlying intrafusal fibers in the equatorial and juxtaequatorial regions. By TEM and HRSEM these endings appeared crescent-shaped and were enveloped by external laminae. Each profile contained a plethora of mitochondria and cytoskeletal organelles. The methodology used in this study provides, for the first time, a three-dimensional view of the exquisite cytological architecture of this neuromuscular receptor. / Medicine, Faculty of / Graduate
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Antiviral Activity of Favipiravir (T-705) Against Lethal Rift Valley Fever Virus Infection in HamstersScharton, Dionna 01 May 2014 (has links)
Rift Valley Fever is a zoonotic, arthropod-borne disease that adversely affects ungulates and people. The etiologic agent, Rift Valley fever virus (RVFV; Bunyaviridae, Phlebovirus), is primarily transmitted through mosquito bites, yet can be transmitted by exposure to infectious aerosols. Presently, there are no licensed vaccines or therapeutics to prevent or treat severe RVFV infection in humans. We have previously reported on the activity of favipiravir (T-705) against the MP-12 vaccine strain of RVFV and other bunyaviruses in cell culture. Additionally, efficacy has been documented in mouse and hamster models of infection with the related Punta Toro virus. Here, we characterize a hamster RVFV challenge model and use it to evaluate the activity of favipiravir against the highly pathogenic ZH501 strain of the virus. Subcutaneous RVFV challenge resulted in substantial serum and tissue viral loads and caused severe disease and mortality within 2-3 days after infection. Oral favipiravir (200 mg/kg/day) prevented mortality in 60% or greater in hamsters challenged with RVFV when administered within 6 h post-exposure and reduced RVFV titers in serum and tissues relative to the time of treatment initiation. In contrast, although ribavirin (75 mg/kg/day) was effective at protecting animals from the peracute RVFV disease, most ultimately succumbed from a delayed-onset neurologic disease associated with high RVFV burden in the brain observed in moribund animals. When combined, T-705 and ribavirin treatment started 24 h post-infection significantly improved survival outcome and reduced serum and tissue virus titers compared to monotherapy. Our findings demonstrate significant post-RVFV exposure efficacy with favipiravir against both peracute disease and delayed-onset neuroinvasion, and suggest added benefit when combined with ribavirin.
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Effects of cadmium on hamster alveolar macrophage function /Somers, Scott Douglas January 1981 (has links)
No description available.
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Plasma total cholesterol and triglyceride responses of hamsters fed oat bran and pinto bean dietsCross, Teresa Jane 05 September 2009 (has links)
The effect of a 53% oat bran diet and a 30% pinto bean diet on hamster plasma total cholesterol (TC) and triglycerides (TG) was investigated. Hamsters were made hypercholesterolemic (average value = 206 mg/dL) and then fed one of four experimental diets, the hypercholesterolemic control (HC), an insoluble fiber (alphacel) control (FC), the oat bran (OB), or the pinto bean (PB) diet for three weeks, with the latter three containing 8.5%, 10.0%, and 7.6%, total dietary fiber, respectively. Plasma TC and TG were measured for each animal before and after the experimental diets. At the end of the experimental period, plasma TC levels of hamsters fed the OB diet (179 mg/dL) were significantly lower than those fed either the HC (203 mg/dL, p<0.05) or FC (221 mg/dL, p<0.001) diets. Plasma TG levels of hamsters fed the OB diet (200 mg/dL) were significantly lower than those fed the FC diet (358 mg/dL, p<0.01). Thus, it was concluded that oat bran significantly lowered plasma TC and TG in hypercholesterolemic hamsters, while pinto beans did not. / Master of Science
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"Imunoglobulina na patogenia da leishmaniose visceral em hamsteres" / Immunoglobulin in the pathogenesis in visceral leishmaniasis in hamstersMathias, Regiane 21 January 2005 (has links)
A patogênese das lesões teciduais na leishmaniose visceral (LV) foi pesquisada em hamsteres infectados com amastigotas de Leishmania (Leishmania.) chagasi. Foi observada a internalização de IgG de hamsteres com LV por células endoteliais da veia umbilical humana in vitro e no fígado e rim, sob microscopia eletrônica de transmissão aos 30 e 60 dias de infecção. Também foi observado o aumento na permeabilidade vascular aos 60 dias de infecção e a IgG purificada de hamsteres com LV induziu aumento na permeabilidade em hamsteres normais. Os resultados sugerem a internalização de IgG por células endoteliais como um mecanismo alternativo envolvido na patogênese das lesões teciduais em LV. / Pathogenesis of tissue lesions in visceral leishmaniasis (VL) was searched in hamsters infected with Leishmania (Leishmania) chagasi amastigotes. Internalization of IgG from VL hamsters by human umbilical vein endothelial cells was observed in vitro and in liver and kidney in hamsters VL, under transmission electron microscopy, at 30 and 60 days of infection. Increased vascular permeability was observed at 60 days of infection in VL hamsters, and purified IgG from VL hamsters induced permeability increase in normal hamsters. These data suggest the internalization of IgG by endothelial cells as an alternative mechanism involved in the pathogenesis of tissue lesions in VL.
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Efeito da proteína de amaranto (Amaranthus cruentus L. BRS Alegria) na atividade enzimática hepática da HMG-CoA redutase e seu papel no metabolismo lipídico em hamsters / Effect of amaranth (Amaranthus cruentus L. BRS Alegria) protein in hepatic enzymatic activity of HMG-CoA reductase and its role in lipid metabolism in hamstersSuraty, Thaís Rezende 30 January 2013 (has links)
Introdução: Atualmente as Doenças Crônicas não Transmissíveis (DCNTs) são um dos maiores problemas de saúde pública da sociedade. É bastante claro o papel da dieta no controle do colesterol e na incidência de doenças cardiovasculares. Neste sentido, o amaranto desperta grande interesse devido a sua propriedade hipocolesterolemizante. Estudos sugerem que seu efeito hipocolesterolemizante está associado à inibição da enzima HMG-CoA redutase, chave na síntese do colesterol endógeno. Objetivo: Avaliar a atividade enzimática hepática da HMG-CoA redutase de hamsters alimentados com proteína de amaranto. Metodologia: Trinta hamsters foram divididos em 5 grupos e receberam dieta diferenciadas pela fonte protéica. Os grupos I e Icol receberam dieta com 20% de proteína de amaranto e os grupos caseína C e Ccol receberam dieta com 20% de caseína. Os grupos \"col\" apresentavam dieta com 0,1% de colesterol e 13,5% de gordura de coco. O metabolismo lipídico foi acompanhado através do monitoramento das concentrações plasmáticas de colesterol total, triacilgliceróis, HDL, e fração não-HDL nos animais. A excreção de colesterol e ácidos biliares foram quantificados nas fezes dos animais e o grau de esteatose hepática foi determinada através de análises histológicas do lobo direito do fígado. A atividade da enzima HMGR nos fígados foi medida por meio do Kit CS 1090 da Sigma-Aldrich com adaptações segundo Cong et al, 2012. A análise é baseada em espectrometria com absorbância de 340nm a 37ºC, que representa a oxidação de NADPH pela HMG-CoA redutase, na presença do substrato HMG-CoA. Conclusões: A proteína de amaranto pode ser considerado um aliado na redução dos agravos gerados pela dislipidemia, uma vez que reduziu significativamente os níveis de colesterol plasmático e gordura hepática, além de ser demonstrado seu efeito na redução da atividade da enzima HMG-CoA redutase dos animais hipercolesterolemizados que se alimentaram com proteína de amaranto. Uma vez verificado o efeito hipocolesterolemizante e seu possível mecanismo de ação por meio da enzima HMG-CoA redutase, espera-se com isso, estimular o consumo pela população brasileira produção de amaranto no Brasil, como alternativa para diversificar a dieta e a agricultura. / Introduction: Nowadays, Non-Communicable Chronic Diseases (NCCD) are a major challenge in health public. It is evident the role of diet in the control of cholesterol and incidence of cardiovascular disease. In this sense, amaranth arouses great interest due to its hypocholesterolemic property. Studies suggest that amaranth\'s hypocholesterolemic effect is associated with the inhibition of the enzyme HMG-CoA reductase, known as the key process to the endogenous cholesterol synthesis. Objective: Evaluate the hepatic enzymatic activity of HMG-CoA reductase in hamsters fed with amaranth protein. Methodology: Amaranth protein was isolated according to the conventional isoelectric precipitation methodology. Thirty hamsters were divided in 5 groups and were fed diets with different protein source. Experimental groups (I and lcol) had a diet containing 20% of protein amaranth and control groups(C and Cool) received a diet with 20% of casein. Moreover, groups \"col\" had also a diet with 0.1% cholesterol and 13.5% coconut oil in their composition. The lipid metabolism was accompanied through monitoring of plasma concentrations of total cholesterol, triglycerides, HDL and non-HDL fraction in animals. Excretion of cholesterol and bile acids were quantified in the feces of animals and the degree of hepatic steatosis was determined by histological analysis of the liver\'s right lobe. The HMGR enzyme activity in the liver was measured by the CS 1090 Kit from Sigma-Aldrich adjusted in accordance with Cong et al, 2012. The analysis is based on spectrometry with absorbance of 340nm at 37 ° C, which represents the oxidation of NADPH by HMG-CoA reductase in the presence of HMG-CoA substrate. Conclusions: Amaranth protein can be considered as an ally in reducing of injuries generated by dyslipidemia, since it significantly reduced levels of plasma cholesterol and hepatic fat. Furthermore, it was demonstrated its effect on reducing activity of HMG-CoA reductase enzyme in hypercholesterolemic animals, which were fed with amaranth protein. Therefore, once verified the hypocholesterolemic effect of amaranth and its possible action mechanism through HMG-CoA reductase enzyme, stimuli on the production of amaranth are expected as an alternative to diversify the diet and agriculture.
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Efeito da proteína de amaranto (Amaranthus cruentus L. BRS Alegria) na atividade enzimática hepática da HMG-CoA redutase e seu papel no metabolismo lipídico em hamsters / Effect of amaranth (Amaranthus cruentus L. BRS Alegria) protein in hepatic enzymatic activity of HMG-CoA reductase and its role in lipid metabolism in hamstersThaís Rezende Suraty 30 January 2013 (has links)
Introdução: Atualmente as Doenças Crônicas não Transmissíveis (DCNTs) são um dos maiores problemas de saúde pública da sociedade. É bastante claro o papel da dieta no controle do colesterol e na incidência de doenças cardiovasculares. Neste sentido, o amaranto desperta grande interesse devido a sua propriedade hipocolesterolemizante. Estudos sugerem que seu efeito hipocolesterolemizante está associado à inibição da enzima HMG-CoA redutase, chave na síntese do colesterol endógeno. Objetivo: Avaliar a atividade enzimática hepática da HMG-CoA redutase de hamsters alimentados com proteína de amaranto. Metodologia: Trinta hamsters foram divididos em 5 grupos e receberam dieta diferenciadas pela fonte protéica. Os grupos I e Icol receberam dieta com 20% de proteína de amaranto e os grupos caseína C e Ccol receberam dieta com 20% de caseína. Os grupos \"col\" apresentavam dieta com 0,1% de colesterol e 13,5% de gordura de coco. O metabolismo lipídico foi acompanhado através do monitoramento das concentrações plasmáticas de colesterol total, triacilgliceróis, HDL, e fração não-HDL nos animais. A excreção de colesterol e ácidos biliares foram quantificados nas fezes dos animais e o grau de esteatose hepática foi determinada através de análises histológicas do lobo direito do fígado. A atividade da enzima HMGR nos fígados foi medida por meio do Kit CS 1090 da Sigma-Aldrich com adaptações segundo Cong et al, 2012. A análise é baseada em espectrometria com absorbância de 340nm a 37ºC, que representa a oxidação de NADPH pela HMG-CoA redutase, na presença do substrato HMG-CoA. Conclusões: A proteína de amaranto pode ser considerado um aliado na redução dos agravos gerados pela dislipidemia, uma vez que reduziu significativamente os níveis de colesterol plasmático e gordura hepática, além de ser demonstrado seu efeito na redução da atividade da enzima HMG-CoA redutase dos animais hipercolesterolemizados que se alimentaram com proteína de amaranto. Uma vez verificado o efeito hipocolesterolemizante e seu possível mecanismo de ação por meio da enzima HMG-CoA redutase, espera-se com isso, estimular o consumo pela população brasileira produção de amaranto no Brasil, como alternativa para diversificar a dieta e a agricultura. / Introduction: Nowadays, Non-Communicable Chronic Diseases (NCCD) are a major challenge in health public. It is evident the role of diet in the control of cholesterol and incidence of cardiovascular disease. In this sense, amaranth arouses great interest due to its hypocholesterolemic property. Studies suggest that amaranth\'s hypocholesterolemic effect is associated with the inhibition of the enzyme HMG-CoA reductase, known as the key process to the endogenous cholesterol synthesis. Objective: Evaluate the hepatic enzymatic activity of HMG-CoA reductase in hamsters fed with amaranth protein. Methodology: Amaranth protein was isolated according to the conventional isoelectric precipitation methodology. Thirty hamsters were divided in 5 groups and were fed diets with different protein source. Experimental groups (I and lcol) had a diet containing 20% of protein amaranth and control groups(C and Cool) received a diet with 20% of casein. Moreover, groups \"col\" had also a diet with 0.1% cholesterol and 13.5% coconut oil in their composition. The lipid metabolism was accompanied through monitoring of plasma concentrations of total cholesterol, triglycerides, HDL and non-HDL fraction in animals. Excretion of cholesterol and bile acids were quantified in the feces of animals and the degree of hepatic steatosis was determined by histological analysis of the liver\'s right lobe. The HMGR enzyme activity in the liver was measured by the CS 1090 Kit from Sigma-Aldrich adjusted in accordance with Cong et al, 2012. The analysis is based on spectrometry with absorbance of 340nm at 37 ° C, which represents the oxidation of NADPH by HMG-CoA reductase in the presence of HMG-CoA substrate. Conclusions: Amaranth protein can be considered as an ally in reducing of injuries generated by dyslipidemia, since it significantly reduced levels of plasma cholesterol and hepatic fat. Furthermore, it was demonstrated its effect on reducing activity of HMG-CoA reductase enzyme in hypercholesterolemic animals, which were fed with amaranth protein. Therefore, once verified the hypocholesterolemic effect of amaranth and its possible action mechanism through HMG-CoA reductase enzyme, stimuli on the production of amaranth are expected as an alternative to diversify the diet and agriculture.
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Perfil lipídico na leishmaniose visceral em hamster e expressão de mRNA de genes relacionados ao metabolismo liprotéico / Lipid profile in visceral leishmaniasis in hamster and expression of mRNA of genes related to lipoprotein metabolismDantas, Ive Maíra de Carvalho 30 January 2014 (has links)
Na fase ativa da leishmaniose visceral (LV) ocorrem alterações no metabolismo de lipoproteínas com redução dos níveis de HDL e aumento de triglicérides. A partir desses dados, focamos neste projeto essas alterações na progressão da infecção e apontamos alguns elementos como seus possíveis desencadeantes. Como essas alterações poderiam resultar de redução de atividade e expressão da lipoproteína lipase (LPL), do receptor alfa do proliferador ativado de peroxissoma (PPAR?) e da proteína transferidora de ésteres de colesteril (CETP), a sua expressão foi avaliada durante a progressão da LV em hamster. Em hamsteres infectados com 2 x 107 amastigotas de L. (L.) infantum observamos aumento de triglicérides nos hamsteres com 55 dias (mediana = 294,0 mg/dL) e 90 dias (303,0 mg/dL ) de infecção comparados aos controles de 55 dias (119,0 mg/dL) e de 90 dias (117,0 mg/dL) (p <= 0,05). Os níveis de colesterol total e de HDL não apresentaram diferença significante entre controles e infectados com 30, 55 e 90 dias de infecção. A expressão de mRNA de PPAR? no fígado com 55 e 90 dias de infecção apresentou tendência de redução nos infectados. Já de CETP no fígado dos hamsteres com 55 dias de infecção, a expressão relativa (CT) estava reduzida nos infectados (0,08) comparados aos controles (1,69) (p <= 0,05) e de LPL no coração dos hamsteres com 90 dias de infecção também estava reduzida (1,43) com relação aos controles (2,61) (p <= 0,05). Há dados na literatura sugerindo a importância de lipídios para o desenvolvimento de amastigotas no hospedeiro vertebrado e é possível que as alterações dos níveis de lipoproteínas contribuam na progressão da infecção. Assim, avaliamos neste estudo o efeito da droga hipolipemiante ciprofibrato no controle do parasitismo na LV em hamster, sabendo-se que ciprofibratos atuam aumentando a expressão de PPAR? e a produção e atividade de LPL. O tratamento com ciprofibrato nos hamsteres com 55 dias de infecção gerou redução de triglicérides (123,0 mg/dL) em relação aos infectados não tratados (294,0 g/dL) (p <= 0,05), além dos níveis de triglicérides nos animais infectados não tratados terem aumentado quando comparados aos controles não tratados (119,0 mg/dL) (p <= 0,05). Houve também, redução de triglicérides nos animais não infectados tratados com ciprofibrato (89,0 mg/dL) comparando-se aos infectados não tratados (p <= 0,05). Os níveis de colesterol nos hamsteres não infectados tratados com ciprofibrato reduziram (53,5 mg/dL) em comparação aos infectados não tratados (93,0 mg/dL) (p <= 0,05). Já naqueles que foram infectados e tratados com ciprofibrato, constatamos redução de colesterol (53,5 mg/dL) quando comparados aos infectados não tratados (p <= 0,05). Os níveis de HDL não aumentaram com ciprofibrato e foram similares entre os hamsteres infectados não tratados e os controles não tratados. A carga parasitária no baço e no fígado não foi reduzida com ciprofibrato. Na leishmaniose visceral em hamster ocorrem alterações do metabolismo lipídico com aumento de triglicérides e redução da expressão da mRNA de LPL e CETP. O tratamento com ciprofibrato foi eficaz no controle das alterações de níveis de lipoproteínas. / In the active phase of visceral leishmaniasis (VL) changes occur in lipoprotein me-tabolism with reduction in HDL and increase in triglyceride (TG) levels. From these data, in this project we focused these changes during the progression of the infection and we approached some elements as their underlying factors. Since these changes may result from the reduction of the activity and the expression of the lipoprotein lipase (LPL), of the peroxisome proliferator-activated receptor alpha (PPAR?) and of the cholesteryl ester transfer protein (CETP), their expression were evaluated during VL progression in hamster. In 2 x 107 L. (L.) infantum amastigote-infected hamsters we observed an increase in the triglycerides in hamsters with 55 days (median = 294.0 mg/dL) and 90 days (303.0 mg/dL) of infection compared with controls of 55 days (119.0 mg/dL) and of 90 days (117.0 mg/dL) (p <= 0.05). The total cholesterol and the HDL levels did not present significant differences between control and in-fected groups at 30, 55 and 90 days of infection. The expression of mRNA of the PPAR in the liver with 55 and 90 days of infection tended to be reduced in infected animals. However the relative expression (CT) of CETP in the liver of hamsters with 55 days of infection was signicantly reduced in infected (0.08) compared with control animals (1.69) (p <= 0.05). The relative expression (CT) of LPL in the heart of hamsters with 90 days of infection was also reduced (1.43) in relation to controls (2.61) (p <= 0.05). There are data in the literature suggesting the importance of lipids for the development of amastigotes in vertebrate host and it is possible that the changes in the lipoprotein levels contribute for the infection progression. Therefore, we evaluated in this study the effect of the lipid-lowering drug ciprofibrate in the control of parasitism in VL in the hamster, knowing that ciprofibrate acts increasing the expression of the PPAR? and of the LPL production and activity. The treatment with ciprofibrate in infected hamsters at 55 days lead to the reduction of triglyceride level (123.0 mg/dL) in relation to non-treated infected animals (294.0 g/dL) (p <= 0.05). Further the triglyceride levels in the non-treated infected animals were in-creased when compared with untreated controls (119.0 mg/dL) (p <= 0.05). There was also reduction of triglyceride in ciprofibrate treated-non infected animals (89.0 mg/dL) compared with non-treated infected animals (p <= 0.05). The cholesterol lev-els were reduced in the ciprofibrate-treated non-infected hamsters (53.5 mg/dL) in comparison to the non-treated infected ones (93.0 mg/dL) (p <= 0.05). In the ciprofibrate-treated infected ones we found a reduction of cholesterol level (53.5 mg/dL) when compared with non treated infected animals (p <= 0.05). The HDL lev-els did not increase with ciprofibrate and they were similar between the non-treated infected hamsters and non-treated controls. The parasite load in the spleen and liver were not reduced with ciprofibrate. In the visceral leishmaniasis in hamster changes occur in the lipid metabolism with increase in the triglyceride level and the reduction of expression of mRNA of LPL and CETP. The treatment with ciprofibrate was ef-fective in the control of changes in the lipoprotein levels.
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