Global ETD Search

11	A N-acetilcisteína atenua a progressão da doença renal crônica / N-acetylcysteine attenuates the progression of chronic kidney disease Shimizu, Maria Heloisa Massola 01 December 2005 (has links) Os biomarcadores do estresse oxidativo encontram-se elevados na urina e no plasma dos pacientes renais crônicos. A aldosterona (ALD) contribui para a lesão renal no modelo de rins remanescentes. Objetivos: 1- Determinar o efeito do antioxidante N-acetilcisteína (NAC) sobre a função renal e a aldosterona plasmática de animais com IRC. 2- Avaliar o efeito da NAC sobre a evolução da IRC, mesmo quando administrada tardiamente. 3- Avaliar os efeitos da NAC associada a Espironolactona (Spi). Material e Métodos: Ratos adultos Wistar machos foram submetidos a nefrectomia de 5/6 (Nx). No estudo 1: Animais foram tratados ou não com NAC na dose de (600mg/l na água de beber) iniciado 7dias após nefrectomia (Nx). Estudos de clearance foram realizados em todos os grupos, 21, 60 e 120 dias após Nx. No estudo 2: 6 animais foram tratados com NAC após 60 dias de Nx e estudados 120 dias após NX. No estudo 3: Os ratos foram tratados com Spi (1.5g/kg de dieta) associados ou não com NAC, ambos iniciados a partir do 7º dia da nefrectomia e estudados 60 dias após a Nx. Em todos os grupos foram avaliados: clearance de inulina (RFG, ml/min/100g peso); proteinúria (Uvpr., mg/24h); aldosterona plasmática (ng/dl); relação potássio/sódio urinário (UK/UNa), pressão arterial (mmHg), TBARS urinário (nmoles/24h) e o índice de glomeruloesclerose (%). Resultados: A ingestão média de NAC foi similar nos respectivos grupos tratados. Significante diminuição de TBARS (marcador de peroxidação lipídica), foi observada nos ratos Nx tratados com NAC (mesmo quando administrado tardiamente). O principal resultado deste estudo foi que a administração de NAC nos animais com nefrectomia de 5/6, protegeu a filtração glomerular (GFR) significativamente, com uma média de clearance de inulina de 0.45 ml/min (50% dos valores normais), mantendose estável 120 dias após a nefrectomia (0,51 ± 0,03). Ao contrário, GFR diminuiu progressivamente nos animais não tratados (0,16 ± 0,03). Nos animais Nx+NAC, a proteinúria, o índice de glomeruloesclerose e a pressão arterial, apresentaram diminuição após 120 dias de Nx e hipertrofia dos corações e das adrenais foram atenuadas. Estes efeitos benéficos estão associados com uma significante redução da aldosterona plasmática e da razão UK/UNa (marcador indireto da ação tubular da aldosterona) e foram observados mesmo com a administração tardia de NAC (60 dias após Nx). A mortalidade foi de 33% no grupo de Nx120, 25% no grupo Nx120+NAC e 10% nos animais Nx120+60NAC. No estudo 3: A espironolactona isoladamente diminuiu a proteinúria dos animais Nx, entretanto, quando associada a NAC promoveu maior proteção da filtração glomerular (Nx60 + NAC+Spi = 0,59±0,04 vs.Nx + 60 + NAC = 0,47 ± 0,05, p < 0,001) e menor pressão arterial (136±2mmHg) do que nos animais tratados apenas com NAC (154 ± 2 mmHg). Conclusões: 1. O antioxidante NAC exerceu efeito protetor sobre a filtração glomerular de ratos com insuficiência renal crônica, mesmo quando administrado tardiamente, além de diminuir as concentrações de aldosterona e TBARS, marcador de peroxidação lipídica. 2. A associação de NAC e espironolactona proporcionou efeito benéfico aditivo sobre a filtração glomerular, acompanhado de uma maior queda da pressão arterial. / Oxidative stress biomarkers are increased in urine and plasma from renal chronic patients. Aldosterone (ALD) contributes to the kidney lesion in the remnant kidney model. Objectives: This studies was carried out to: 1- Determine the effect of antioxidant N-acetylcysteine (NAC) on kidney function and plasma aldosterone on animals with chronic renal failure (CRF); 2- Evaluate the effect of NAC on the CRF evolution, even when administered at a later stage; 3- Evaluate the effects of NAC associated with spironolactone (SPI). Material and Methods: Adult male Wistar rats were submitted to 5/6 nephrectomy (Nx). In study 1: Animals were treated or not with NAC (600 mg/l in drinking water), started 7 days after Nx. Clearance studies were performed on all rats at 21, 60 and 120 days after Nx. In study 2: 6 rats were treated with NAC initiated 60 days after Nx and studied 120 days after Nx. In study 3: rats were treated with Spi (1.5 g/Kg diet) associated or not to NAC, both initiated 7 days after Nx-treated rats and studied 60 days after Nx. In all experiments the following were measured: inulin clearance (GRF, ml/min/100g body weight); proteinuria (Uvpr, mg/24h); plasma aldosterone (ng/dl); urinary potassium/sodium ratio (UK/UNa); blood pressure (mmHg); urinary TBARS (nmoles/24h) and glomerulosclerosis index (%). Results: Mean daily NAC ingestion was similar in respective treated groups. A significant decrease in urinary TBARS (an index of lipid peroxidation) was observed in the NAC treated rats even when administered at a later stage. The main new finding of this study is that NAC administration to 5/6-Nx rats protects the glomerular filtration rate (GFR) significantly, with a mean inulin clearance of 0.45 (50% of the normal values), remaining stable 120 days following nephrectomy (0.51±0.03). Conversely, GFR fell progressively in untreated rats (0.16±0.03). In Nx+NAC rats, proteinuria, glomerulosclerosis index and blood pressure all decreased by day 120, and heart and adrenal hypertrophy were attenuated. These beneficial effects were associated with a significant reduction in plasma aldosterone and urinary sodium/potassium (UK/UNa) ratio (indirect marker of aldosterone tubular action) and were observed even when NAC was administered later (60 days after Nx). Mortality was 33% in the Nx 120 group, 25% in the Nx120+NAC group and 14.3% in the Nx120 (Nx60+60NAC). In study 3: Spironolactone isolatedly decreased proteinuria in the Nx animals, however when associated with NAC it caused more protection of GFR (Nx60+NAC+Spi = 0.59±0.04 vs Nx60+NAC = 0.47 ± 0.05, p < 0.001) and lower blood pressure (136±2 mmHg) than in the animals treated only with NAC (154±2 mmHg). The combination of Spi and NAC lowered blood pressure and improve GFR protection. Conclusion: 1. In the remnant kidney model, NAC has a protective effect attributable to decreased plasma aldosterone and lower of lipid peroxidation indicative of thiobarbituric acid reactive substances (TBARS) lower levels, even in the later stages. 2. Combination of NAC and Spi showed an extra beneficial effect over glomerular filtration, and a higher decrease of blood pressure. Acetilcisteína Acetylcysteine Aldosterona Aldosterone Chronic kidney failure Espironolactona. Insuficiência renal crônica Inulin Inulina Kidney function renal Lipid peroxidation Peroxidação de lipídeos Ratos Wistar Spironolactone Testes de função renal Thiobarbituric acid reactive Wistar rats
12	O impacto de reúso de dialisadores nos marcadores de estresse oxidativo e inflamatórios em pacientes em hemodiálise / Evaluation of oxidative stress and inflamatory markers on hemodialysis patients with and without dialysers reuse Furlan, Carla Barbosa Muraro 27 March 2014 (has links) A morbimortalidade dos pacientes em hemodiálise permanece alta apesar da evolução tecnológica do procedimento, sendo que os eventos cardiovasculares são a sua principal causa. Estes desencadeados pela alta prevalência de fatores de risco tradicionais, fatores relacionados ao procedimento dialítico e estresse oxidativo. Considerando o procedimento dialítico e o estresse oxidativo, foi avaliado o quanto a habitual prática de reuso de dialisadores/RD (difundida nas Américas e amparada principalmente por questões econômicas) e uso único de dialisadores, influenciam nos marcadores inflamatórios e de estresse oxidativo. Para isto, foram utilizados como marcadores laboratoriais as medidas de PCR ultrassensível (u PCR), interleucina 6 (IL6), a determinação de substâncias reativas ao ácido tiobarbitúrico (TBARS), superóxido dismutase (SOD), glutationa (GSH) e albumina, em 29 pacientes em tratamento de hemodiálise. Estes pacientes encontravam-se em tratamento com dialisadores de alto fluxo do tipo polieterssulfona e reuso manual, e ao iniciar este estudo foram programados 3 ciclos sequenciais com duração de 6 semanas com as seguintes características: primeiro ciclo (uso único de dialisadores;); segundo ciclo (reuso de dialisadores); terceiro ciclo (reuso de dialisadores e administração de N-acetilcisteína/NAC, na dose de 1200 mg/dia). Foram coletadas amostras de sangue de cada paciente no início e final da última sessão de hemodiálise anteriormente ao início dos ciclos (denominado Período 1) e no início e final da última sessão de hemodiálise de cada ciclo (denominados Períodos 2, 3 e 4 respectivamente). O TBARS aumentou no período de uso único. Todas as demais variáveis não apresentaram diferença significativa. Os resultados indicaram que o RD pode proporcionar uma melhora no estresse oxidativo. O uso único foi associado com maior estresse oxidativo. Não foi encontrado nenhum benefício adicional com NAC / The morbidity and mortality of patients undergoing hemodialysis remains high despite the technological development of this procedure, and cardiovascular events are the main causes of morbidity and mortality. These cardiovascular events are triggered by the high prevalence of traditional risk factors, factors associated with dialysis procedures, and oxidative stress. Considering the factors associated with dialysis procedures and oxidative stress, we assessed how dialyzer reuse (DR; widespread in the Americas, especially because of economic issues) and use of single-use dialyzers influence oxidative stress and inflammatory markers. We used ultrasensitive PCR (u-PCR) to measure levels of the laboratory markers interleukin-6 (IL6), thiobarbituric acid reactive substances (TBARS), superoxide dismutase (SOD), glutathione (GSH), and albumin in 29 patients undergoing hemodialysis treatment. These patients were receiving treatment with polyethersulfone high-flux dialyzers and manual reuse. In the initial phase of this study, the 3 following sequential cycles, each lasting 6 weeks, were scheduled: first cycle (single-use dialyzers); second cycle (DR); and third cycle (DR and administration of N-acetylcysteine [NAC] at a dose of 1200 mg/day). Blood samples were collected from each patient at the beginning and end of the last hemodialysis session that preceded the start of the cycles (termed Period 1), and at the beginning and end of the last hemodialysis session of each cycle (termed Periods 2, 3, and 4, respectively). The levels of TBARS increased during the single-use period. The remaining variables did not show significant differences. The results indicated that DR may ameliorate oxidative stress. Single-use dialyzers were associated with higher oxidative stress. No additional benefit was found with use of NAC Acetilcisteína/uso terapêutico Acetylcysteine/therapeutic use Ácido peracético Diálise renal Equipment reuse Estresse oxidativo Inflamação Inflammation Oxidative stress Peracetic acid Renal dialysis Reutilização de equipamento Thiobarbituric acid reactive substances
13	OTIMIZAÇÃO DE UMA FORMULAÇÃO DE FISHBURGER DE JUNDIÁ (RHAMDIA QUELEN) VISANDO O APROVEITAMENTO DE RESÍDUOS DA FILETAGEM DO PROCESSAMENTO DE FRUTAS / OPTIMIZATION OF A SILVER CATFISH FISH (RHAMDIA QUELEN) BURGER FORMULATION AIMING AT USING FILLETING WASTES AND FRUIT SEEDS Bochi, Vivian Caetano 23 February 2007 (has links) This work was aimed at optimizing a formulation of silver catfish fishburgers (Rhamdia quelen) using filleting wastes and extract from fruit seeds. The utilization of filleting wastes from silver catfish in the formulation of fishburgers was evaluated by replacing grounded fish fillets with increasing levels (0-control, 20, 50, and 80%) of pulp obtained from filleting wastes (PFW). Fat content of burgers increased with increasing levels of PFW (p<0.05). Burgers with 50-80% PFW had lower n-6/n-3 ratio than control (p<0.05). Fat and moisture retention after cooking were not affected by PFW, while cooking yield increased in burgers with 50% PFW when compared to all other formulations (p<0.05). Texture and juiciness were not affected by PFW. However, burgers containing 80% PFW had lower overall acceptance than controls (p<0.05). Mango (Mangifera indica L.), peach (Prunus persica), and passion fruit (Passiflora sp.) seeds were examined for their total phenolic content, radical scavenging capacity against DPPH (1,1-diphenyl-2-picrylhydrazyl) radicals, ferric-reducing antioxidant power (FRAP), and antioxidant activity against lipid oxidation in a fish model system (0.05, 0.1, 0.15, and 0.3 mg phenolic compounds/4.4ml of silver catfish homogenate). Mango seed extract (MSE) showed the highest phenolic content and total antioxidant activity by DPPH and FRAP assays. Lipid oxidation in fish model system (at 37oC during 90 min) was retarded by the three seed extracts at all concentrations tested. MSE that had the highest antioxidant activity in vitro, was also evaluated against lipid oxidation in fishburgers produced from silver catfish filleting wastes. Burger formulations with 50% pulp from filleting wastes were prepared containing MSE (0, 30, and 90 ppm phenolic compounds) and conjugated dienes, peroxide value, tiobarbituric acid reactive substances, and free fatty acids were the oxidation products measured during frozen storage at -10 and -20oC. All lipid damage measurements were affected by the storage time and temperature. However, after 120 days at both temperatures, TBARS levels of fishburgers did not reach threshold limit for human consumption. MSE had no antioxidant effect against lipid oxidation in silver catfish burgers. Filleting wastes could substitute up to 50% of fish fillets with no changes in sensory acceptance, an improvement of nutritional value, and cooking characteristics, with good lipid stability during at least 120 days of freezing storage. / Este trabalho avaliou o aproveitamento de resíduos resultantes da filetagem e de extratos vegetais de sementes de frutas na otimização de formulações de fishburgers de jundiá (Rhamdia quelen). Os resíduos da filetagem do jundiá foram processados e obteve-se uma polpa de resíduos da filetagem (PRF) utilizada em diferentes níveis (0-controle, 20, 50, e 80%) para substituir os filés de peixe na formulação de fishburger. O teor de gordura aumentou com a utilização de PSF nas formulações (p<0,05). Os fishburgers produzidos com 50-80% PRF apresentaram menores valores para as razões de ácidos graxos n-6/n-3 do que os valores obtidos para o controle (p<0,05). A capacidades de retenção de umidade e de retenção de gordura pós-cocção não foram afetadas pela utilização de PRF, no entanto as formulações com 50% de PRF tiveram os maiores rendimentos pós-cocção (p<0,05). A análise sensorial revelou que a textura e suculência das formulações não foram alteradas pela utilização de PRF, porém a incorporação de 80% de PRF reduziu a aceitação do produto em relação ao controle (p<0,05). Foram determinados, para extratos de sementes de manga (Mangifera indica L.), pêssego (Prunus persica), e maracujá (Passiflora sp.), o conteúdo fenólico, a atividade antioxidante pelos métodos do DPPH (1,1-difenil-2-picrilhidrazil), FRAP (poder antioxidante de redução do ferro) e a capacidade de impedir a oxidação lipídica em um sistema modelo contendo peixe (0,05, 0,1, 0,15 e 0,3 mg de compostos fenólicos/4,4ml de homogeneizado de carne de jundiá). As sementes de manga apresentaram o maior teor de compostos fenólicos totais e atividade antioxidante em DPPH e pelo método de FRAP. A oxidação lipídica no homogeneizado de carne de peixe submetido ao aquecimento (37ºC) por 90 minutos foi impedida pelo extrato das três sementes de frutas em todas as concentrações testadas. O extrato de semente de manga, que apresentou a maior atividade antioxidante in vitro, foi escolhido para a avaliação de sua capacidade em impedir a oxidação da uma formulação de fishburger produzida com resíduos da filetagem. Foram preparadas formulações de fishburger contendo 50% de resíduos de filetagem e diferentes níveis de extrato de semente de manga (0, 30 e 90 ppm de compostos fenólicos) que foram armazenadas a -10 ou -20 oC. A oxidação lipídica durante o congelamento foi acompanhada determinando-se os teores de dienos conjugados, valor de peróxidos, substâncias reativas ao ácido tiobarbitúrico e ácidos graxos livres. Todas as medidas de oxidação lipídica foram afetadas pela temperatura e tempo de estocagem. No entanto, ao final de 120 dias, os níveis de TBARS não alcançaram o valor limite para consumo humano. O extrato de semente de manga não apresentou efeito antioxidante contra a peroxidação lipídica nas formulações de fishburgers de jundiá. A substituição de filé de jundiá por polpa de resíduos da filetagem pode ser realizada até o nível de 50% na formulação de fishburger de jundiá significativas na qualidade sensorial, resultando em produtos com melhor valor nutricional e características pós-cocção, estáveis durante pelo menos 120 dias de congelamento. Composição de ácidos graxos Oxidação lipídica Pêssego Maracujá Manga Fatty acid composition Lipid oxidation Peach Passion fruit Mango Thiobarbituric acid reactive substances
14	A N-acetilcisteína atenua a progressão da doença renal crônica / N-acetylcysteine attenuates the progression of chronic kidney disease Maria Heloisa Massola Shimizu 01 December 2005 (has links) Os biomarcadores do estresse oxidativo encontram-se elevados na urina e no plasma dos pacientes renais crônicos. A aldosterona (ALD) contribui para a lesão renal no modelo de rins remanescentes. Objetivos: 1- Determinar o efeito do antioxidante N-acetilcisteína (NAC) sobre a função renal e a aldosterona plasmática de animais com IRC. 2- Avaliar o efeito da NAC sobre a evolução da IRC, mesmo quando administrada tardiamente. 3- Avaliar os efeitos da NAC associada a Espironolactona (Spi). Material e Métodos: Ratos adultos Wistar machos foram submetidos a nefrectomia de 5/6 (Nx). No estudo 1: Animais foram tratados ou não com NAC na dose de (600mg/l na água de beber) iniciado 7dias após nefrectomia (Nx). Estudos de clearance foram realizados em todos os grupos, 21, 60 e 120 dias após Nx. No estudo 2: 6 animais foram tratados com NAC após 60 dias de Nx e estudados 120 dias após NX. No estudo 3: Os ratos foram tratados com Spi (1.5g/kg de dieta) associados ou não com NAC, ambos iniciados a partir do 7º dia da nefrectomia e estudados 60 dias após a Nx. Em todos os grupos foram avaliados: clearance de inulina (RFG, ml/min/100g peso); proteinúria (Uvpr., mg/24h); aldosterona plasmática (ng/dl); relação potássio/sódio urinário (UK/UNa), pressão arterial (mmHg), TBARS urinário (nmoles/24h) e o índice de glomeruloesclerose (%). Resultados: A ingestão média de NAC foi similar nos respectivos grupos tratados. Significante diminuição de TBARS (marcador de peroxidação lipídica), foi observada nos ratos Nx tratados com NAC (mesmo quando administrado tardiamente). O principal resultado deste estudo foi que a administração de NAC nos animais com nefrectomia de 5/6, protegeu a filtração glomerular (GFR) significativamente, com uma média de clearance de inulina de 0.45 ml/min (50% dos valores normais), mantendose estável 120 dias após a nefrectomia (0,51 ± 0,03). Ao contrário, GFR diminuiu progressivamente nos animais não tratados (0,16 ± 0,03). Nos animais Nx+NAC, a proteinúria, o índice de glomeruloesclerose e a pressão arterial, apresentaram diminuição após 120 dias de Nx e hipertrofia dos corações e das adrenais foram atenuadas. Estes efeitos benéficos estão associados com uma significante redução da aldosterona plasmática e da razão UK/UNa (marcador indireto da ação tubular da aldosterona) e foram observados mesmo com a administração tardia de NAC (60 dias após Nx). A mortalidade foi de 33% no grupo de Nx120, 25% no grupo Nx120+NAC e 10% nos animais Nx120+60NAC. No estudo 3: A espironolactona isoladamente diminuiu a proteinúria dos animais Nx, entretanto, quando associada a NAC promoveu maior proteção da filtração glomerular (Nx60 + NAC+Spi = 0,59±0,04 vs.Nx + 60 + NAC = 0,47 ± 0,05, p < 0,001) e menor pressão arterial (136±2mmHg) do que nos animais tratados apenas com NAC (154 ± 2 mmHg). Conclusões: 1. O antioxidante NAC exerceu efeito protetor sobre a filtração glomerular de ratos com insuficiência renal crônica, mesmo quando administrado tardiamente, além de diminuir as concentrações de aldosterona e TBARS, marcador de peroxidação lipídica. 2. A associação de NAC e espironolactona proporcionou efeito benéfico aditivo sobre a filtração glomerular, acompanhado de uma maior queda da pressão arterial. / Oxidative stress biomarkers are increased in urine and plasma from renal chronic patients. Aldosterone (ALD) contributes to the kidney lesion in the remnant kidney model. Objectives: This studies was carried out to: 1- Determine the effect of antioxidant N-acetylcysteine (NAC) on kidney function and plasma aldosterone on animals with chronic renal failure (CRF); 2- Evaluate the effect of NAC on the CRF evolution, even when administered at a later stage; 3- Evaluate the effects of NAC associated with spironolactone (SPI). Material and Methods: Adult male Wistar rats were submitted to 5/6 nephrectomy (Nx). In study 1: Animals were treated or not with NAC (600 mg/l in drinking water), started 7 days after Nx. Clearance studies were performed on all rats at 21, 60 and 120 days after Nx. In study 2: 6 rats were treated with NAC initiated 60 days after Nx and studied 120 days after Nx. In study 3: rats were treated with Spi (1.5 g/Kg diet) associated or not to NAC, both initiated 7 days after Nx-treated rats and studied 60 days after Nx. In all experiments the following were measured: inulin clearance (GRF, ml/min/100g body weight); proteinuria (Uvpr, mg/24h); plasma aldosterone (ng/dl); urinary potassium/sodium ratio (UK/UNa); blood pressure (mmHg); urinary TBARS (nmoles/24h) and glomerulosclerosis index (%). Results: Mean daily NAC ingestion was similar in respective treated groups. A significant decrease in urinary TBARS (an index of lipid peroxidation) was observed in the NAC treated rats even when administered at a later stage. The main new finding of this study is that NAC administration to 5/6-Nx rats protects the glomerular filtration rate (GFR) significantly, with a mean inulin clearance of 0.45 (50% of the normal values), remaining stable 120 days following nephrectomy (0.51±0.03). Conversely, GFR fell progressively in untreated rats (0.16±0.03). In Nx+NAC rats, proteinuria, glomerulosclerosis index and blood pressure all decreased by day 120, and heart and adrenal hypertrophy were attenuated. These beneficial effects were associated with a significant reduction in plasma aldosterone and urinary sodium/potassium (UK/UNa) ratio (indirect marker of aldosterone tubular action) and were observed even when NAC was administered later (60 days after Nx). Mortality was 33% in the Nx 120 group, 25% in the Nx120+NAC group and 14.3% in the Nx120 (Nx60+60NAC). In study 3: Spironolactone isolatedly decreased proteinuria in the Nx animals, however when associated with NAC it caused more protection of GFR (Nx60+NAC+Spi = 0.59±0.04 vs Nx60+NAC = 0.47 ± 0.05, p < 0.001) and lower blood pressure (136±2 mmHg) than in the animals treated only with NAC (154±2 mmHg). The combination of Spi and NAC lowered blood pressure and improve GFR protection. Conclusion: 1. In the remnant kidney model, NAC has a protective effect attributable to decreased plasma aldosterone and lower of lipid peroxidation indicative of thiobarbituric acid reactive substances (TBARS) lower levels, even in the later stages. 2. Combination of NAC and Spi showed an extra beneficial effect over glomerular filtration, and a higher decrease of blood pressure. Acetilcisteína Aldosterona Espironolactona. Insuficiência renal crônica Inulina Peroxidação de lipídeos Ratos Wistar Testes de função renal Acetylcysteine Aldosterone Chronic kidney failure Inulin Kidney function renal Lipid peroxidation Spironolactone Thiobarbituric acid reactive Wistar rats
15	Efeito dos carotenóides licopeno e astaxantina sobre danos renais induzidos por cloreto de mercúrio. / Effect of lycopene and astaxanthin carotenoids on renal damage induced by mercuric chloride. Augusti, Paula Rossini 09 March 2007 (has links) Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Mercury is a heavy metal toxic for any living tissue, being kidneys the first target for the inorganic form. Oxidative stress has been pointed as an important molecular mechanism for kidney injury in inorganic mercury poisoning and the interaction of the metal with endogenous thiol-containing molecules, such as δ-aminolevulinate desidratase (δ-ALA-D), seems to contribute to this process. Lycopene and astaxanthin are plentiful carotenoids in tomatoes and algaes and seafoods, respectively. They have been widely studied because of their large antioxidant properties. This work evaluated the ability of lycopene and astaxanthin to prevent HgCl2 toxicity, assessing parameters like δ-ALA-D and glutathione S-transferase (GST) activities, non-protein sulfhydrylic groups content (NPSH), production of thiobarbituric acid reactive substances (TBARS) and activities of antioxidant enzymes like superoxide dismutase (SOD), glutathione peroxidase (GSH-Px), and catalase (CAT), besides creatinine and uric acid plasma levels and histopathological analyses. Adult Wistar rats received lycopene or astaxanthin, by gavage, on doses of 0, 10, 25, or 50 mg/kg, six hours prior to the administration of 0 or 5 mg/kg HgCl2, yielding 8 experimental groups. After twelve hours of exposure to HgCl2 animals were killed. HgCl2 inhibited renal δ-ALA-D activity and increased TBARS levels in kidney and creatinine levels in plasma along with renal tubular necrosis. Lycopene prevented HgCl2-induced inhibition of δ-ALA-D activity and increase of lipid peroxidation in kidney, but not the increase in plasma creatinine levels or renal tubular necrosis caused by HgCl2. Although astaxanthin have not prevented HgCl2-induced inhibition of δ-ALA-D and increase in plasma creatinine levels, this carotenoid prevented lipid peroxidation and attenuated renal tubular necrosis caused by HgCl2. GPx and CAT activities were enhanced, while SOD activity was depressed, in mercury-treated rats when compared to control and these effects were prevented by some lycopene doses and by all astaxanthin doses evaluated. Some doses of lycopene negativelly affected antioxidant enzymes activities per se and the mechanism involved in this response has not been elucidated yet. Neither HgCl2 nor carotenoids treatment changed the content of NPSH groups or GST activity in kidney or uric acid levels in plasma. Our results indicate that although lycopene and astaxanthin did not prevent HgCl2-induced creatinine increase in plasma, changes in the activity of antioxidant enzymes might be limited by the use of these car / O mercúrio é um metal pesado com toxicidade comprovada, capaz de causar danos em qualquer tecido com o qual tenha contato, sendo o rim o principal alvo para sua forma inorgânica. O estresse oxidativo tem sido apontado como um importante mecanismo molecular para a injúria renal induzida por mercúrio inorgânico e a interação desse metal com moléculas contendo grupos sulfidrílicos, tais como a enzima δ-aminolevulinato desidratase (δ-ALA-D), parece contribuir para esse processo. Licopeno e astaxantina são carotenóides abundantes em tomates e em algas e frutos do mar, respectivamente. Ambos têm sido amplamente estudados por suas propriedades antioxidantes. No presente estudo foi avaliado o efeito do licopeno e da astaxantina sobre a toxicidade do HgCl2 em rins de ratos, utilizando-se como parâmetros a atividade das enzimas δ-ALA-D e glutationa Stransferase (GST), quantidade de grupos sulfidrílicos não protéicos (NPSH), produção de substâncias reativas ao ácido tiobarbitúrico (TBARS), atividade das enzimas antioxidantes superóxido dismutase (SOD), glutationa peroxidase (GSH-Px) e catalase (CAT), além dos níveis plasmáticos de creatinina e ácido úrico e análise histopatológica. Ratos Wistar adultos receberam, por gavage, licopeno ou astaxantina nas doses de 0, 10, 25 ou 50 mg/kg, seis horas antes de receberem uma injeção subcutânea de HgCl2 (0 ou 5 mg/kg), resultando assim, em 8 grupos experimentais. Após doze horas da exposição ao HgCl2, os animais foram sacrificados. O HgCl2 inibiu a δ-ALA-D renal, aumentou a produção de TBARS e níveis plasmáticos de creatinina, além de causar necrose tubular. O licopeno preveniu a inibição da δ-ALA-D e a peroxidação lipídica, mas não preveniu o aumento de creatinina no plasma nem a ocorrência de necrose tubular induzidos pelo HgCl2. Embora a astaxantina não tenha prevenido a inibição da δ-ALA-D e o aumento nos níveis plasmáticos de creatinina, este carotenóide preveniu a ocorrência da peroxidação lipídica e atenuou a necrose tubular causada pelo HgCl2. As atividades das enzimas GSH-Px e CAT aumentaram, enquanto a atividade da SOD diminuiu nos animais tratados com HgCl2 e esses efeitos foram prevenidos por algumas doses de licopeno e por todas as doses de astaxantina avaliadas. Algumas doses de licopeno tiveram efeito negativo sobre as enzimas antioxidantes per se e o mecanismo envolvido nessa resposta ainda não foi elucidado. O tratamento com HgCl2 ou carotenóides não alterou o conteúdo de NPSH ou a atividade da GST no tecido renal, nem os níveis plasmáticos de ácido úrico. Os resultados indicam que embora licopeno e astaxantina não tenham prevenido o aumento nos níveis plasmáticos de creatinina induzido por HgCl2, as alterações nas enzimas antioxidantes podem ser limitadas pelo uso destes carotenóides. δ-aminolevulinato desidratase Enzimas antioxidantes Necrose tubular Ratos D-aminolevulinate dehydratase Antioxidant enzymes Tubular necrosis Rats Thiobarbituric acid reactive substances CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA
16	O impacto de reúso de dialisadores nos marcadores de estresse oxidativo e inflamatórios em pacientes em hemodiálise / Evaluation of oxidative stress and inflamatory markers on hemodialysis patients with and without dialysers reuse Carla Barbosa Muraro Furlan 27 March 2014 (has links) A morbimortalidade dos pacientes em hemodiálise permanece alta apesar da evolução tecnológica do procedimento, sendo que os eventos cardiovasculares são a sua principal causa. Estes desencadeados pela alta prevalência de fatores de risco tradicionais, fatores relacionados ao procedimento dialítico e estresse oxidativo. Considerando o procedimento dialítico e o estresse oxidativo, foi avaliado o quanto a habitual prática de reuso de dialisadores/RD (difundida nas Américas e amparada principalmente por questões econômicas) e uso único de dialisadores, influenciam nos marcadores inflamatórios e de estresse oxidativo. Para isto, foram utilizados como marcadores laboratoriais as medidas de PCR ultrassensível (u PCR), interleucina 6 (IL6), a determinação de substâncias reativas ao ácido tiobarbitúrico (TBARS), superóxido dismutase (SOD), glutationa (GSH) e albumina, em 29 pacientes em tratamento de hemodiálise. Estes pacientes encontravam-se em tratamento com dialisadores de alto fluxo do tipo polieterssulfona e reuso manual, e ao iniciar este estudo foram programados 3 ciclos sequenciais com duração de 6 semanas com as seguintes características: primeiro ciclo (uso único de dialisadores;); segundo ciclo (reuso de dialisadores); terceiro ciclo (reuso de dialisadores e administração de N-acetilcisteína/NAC, na dose de 1200 mg/dia). Foram coletadas amostras de sangue de cada paciente no início e final da última sessão de hemodiálise anteriormente ao início dos ciclos (denominado Período 1) e no início e final da última sessão de hemodiálise de cada ciclo (denominados Períodos 2, 3 e 4 respectivamente). O TBARS aumentou no período de uso único. Todas as demais variáveis não apresentaram diferença significativa. Os resultados indicaram que o RD pode proporcionar uma melhora no estresse oxidativo. O uso único foi associado com maior estresse oxidativo. Não foi encontrado nenhum benefício adicional com NAC / The morbidity and mortality of patients undergoing hemodialysis remains high despite the technological development of this procedure, and cardiovascular events are the main causes of morbidity and mortality. These cardiovascular events are triggered by the high prevalence of traditional risk factors, factors associated with dialysis procedures, and oxidative stress. Considering the factors associated with dialysis procedures and oxidative stress, we assessed how dialyzer reuse (DR; widespread in the Americas, especially because of economic issues) and use of single-use dialyzers influence oxidative stress and inflammatory markers. We used ultrasensitive PCR (u-PCR) to measure levels of the laboratory markers interleukin-6 (IL6), thiobarbituric acid reactive substances (TBARS), superoxide dismutase (SOD), glutathione (GSH), and albumin in 29 patients undergoing hemodialysis treatment. These patients were receiving treatment with polyethersulfone high-flux dialyzers and manual reuse. In the initial phase of this study, the 3 following sequential cycles, each lasting 6 weeks, were scheduled: first cycle (single-use dialyzers); second cycle (DR); and third cycle (DR and administration of N-acetylcysteine [NAC] at a dose of 1200 mg/day). Blood samples were collected from each patient at the beginning and end of the last hemodialysis session that preceded the start of the cycles (termed Period 1), and at the beginning and end of the last hemodialysis session of each cycle (termed Periods 2, 3, and 4, respectively). The levels of TBARS increased during the single-use period. The remaining variables did not show significant differences. The results indicated that DR may ameliorate oxidative stress. Single-use dialyzers were associated with higher oxidative stress. No additional benefit was found with use of NAC Acetilcisteína/uso terapêutico Ácido peracético Diálise renal Estresse oxidativo Inflamação Reutilização de equipamento Acetylcysteine/therapeutic use Equipment reuse Inflammation Oxidative stress Peracetic acid Renal dialysis Thiobarbituric acid reactive substances
17	Antioxidant properties of Lippia javanica (Burm.f.) Spreng. / C. Pretorius Pretorius, Corlea January 2010 (has links) The evolution of aerobic metabolic processes unavoidably led to the production of reactive oxygen species (ROS). ROS have the ability to cause harmful oxidative damage to biomolecules. Increased ROS generation and subsequent oxidative stress have been associated with aging and neurodegenerative disorders such as Parkinson’s and Alzheimer’s diseases as a result of the extreme sensitivity of the central nervous system to damage from ROS. Antioxidant defence systems have co–evolved with aerobic metabolic processes to counteract oxidative damage inflicted by ROS. The impact of neurodegenerative disorders on society is increasing rapidly as the life expectancy of the global population increases. In this day and age, a much younger group of the population is also experiencing neurodegenerative symptoms as a result of the harmful effect of the human immunodeficiency virus (HIV) on the central nervous system. Plants are an invaluable source of medicinal compounds. The use of plants for their healing properties is rooted in ancient times. The aim of this study was to select from twenty one plants, the plant with the most promising antioxidant activity and to determine whether extracts of this plant could act as free radical scavengers, comparing the results to Trolox, a known free radical scavenger. The next step was to isolate and characterize a compound from an extract exhibiting promising antioxidant activity. Bioassay–guided fractionation was followed to achieve this. During screening trials, twenty one plants, namely Berula erecta, Heteromorpha arborescens, Tarchonanthus camphoratus, Vernonia oligocephala, Gymnosporia buxifolia, Acacia karroo, Elephantorrhiza elephantina, Erythrina zeyheri, Leonotis leonurus, Plectranthus ecklonii, P. rehmanii, P. venteri, Salvia auretia, S. runcinata, Solenostemon latifolius, S. rotundifolius, Plumbago auriculata, Clematis brachiata, Vangueria infausta, Physalis peruviana and Lippia javanica were selected from literature, based on reported antioxidant activity within the plant families, for screening of their antioxidant activity. One hundred and ten extracts were prepared from the leaves, using Soxhlet extraction and the solvents petroleum ether (PE), dichloromethane (DCM), ethyl acetate (EtOAc) and ethanol (EtOH), consecutively. The focus during initial screening trials was on chemistry–based assays. The oxygen radical absorbance capacity (ORAC) and ferric reducing antioxidant power (FRAP) assays were employed for the primary screening of the one hundred and ten leaf extracts. The ORAC assay was used to determine whether the plant extracts were able to scavenge peroxyl radicals and the FRAP assay was used to determine the reducing abilities of the extracts. Quantification of the peroxyl radical scavenging activity by the ORAC assay revealed that activity was observed for most of the extracts, with the ethyl acetate and ethanol extracts of L. javanica exhibiting the most promising activity. This pattern of activity was also found with the reducing capacity evaluated by the FRAP assay in which the EtOAc and EtOH extracts of L. javanica also exhibited the most promising activity. L. javanica was selected for further study by screening for biological activity, employing the nitro–blue tetrazolium (NBT) assay and thiobarbituric acid reactive substances (TBARS) assay. Using a cyanide model to induce neurotoxic effects in rat brain homogenate, the neuroprotective properties of the extracts of L. javanica leaves were examined using the NBT assay and compared to that of Trolox. The NBT assay determines the level of superoxide anions. All the extracts of L. javanica significantly reduced superoxide anion generation at all concentrations used. The petroleum ether and ethyl acetate extracts, at all concentrations, reduced superoxide anion generation to values lower than that of the control, suggesting that these extracts may be able to attenuate normal free radical processes in the brain. The petroleum ether extract exhibited the most promising activity at a concentration of 1.25 and 2.5 mg/ml and also exhibited similar results as the ethyl acetate extract at a lower concentration than the ethyl acetate extract (2.5 mg/ml compared to 5 mg/ml). A toxin–solution consisting of hydrogen peroxide (H2O2), iron(III)chloride (FeCl3) and ascorbic acid was used to induce lipid peroxidation and the ability of the extracts of the leaves of L. javanica to attenuate lipid peroxidation was investigated in rat brain homogenate and compared to that of Trolox. All of the extracts of L. javanica significantly attenuated toxininduced lipid peroxidation at all concentrations used. All of the extracts were also able to significantly attenuate toxin–induced lipid peroxidation to values lower than that of the control. These results suggest that all of the extracts of L. javanica possess the ability to attenuate not only toxin–induced lipid peroxidation, but also lipid peroxidation that occurs during normal processes in the brain. The petroleum ether extract was subjected to bioassay–guided fractionation using column and thin–layer chromatography and the NBT and TBARS assays. Fraction DD1 was investigated by means of nuclear magnetic resonance, infrared and mass spectrometry. The exact structure of fraction DD1 was not elucidated. Considering all the results, it is clear that L. javanica shows great potential as a medicinal plant with antioxidant activity and may therefore be beneficial in diminishing the destructive oxidative effects inflicted by free radicals. There are however still many compounds to be isolated from L. javanica. Key words: Verbenaceae, Lippia javanica, antioxidant, neurodegeneration, oxygen radical absorbance capacity (ORAC), ferric reducing antioxidant power (FRAP), nitro–blue tetrazolium assay (NBT), thiobarbituric acid reactive substances assay (TBARS). / Thesis (M.Sc. (Pharmaceutical Chemistry))--North-West University, Potchefstroom Campus, 2011. Verbenaceae Lippia javanica Antioxidant Neurodegeneration Ferric reducing antioxidant power (FRAP) Nitro-blue tetrazolium assay (NBT) Anti-oksidant Neurodegenerasie Nitrobloutetrasolium toets (NBT)
18	Antioxidant properties of Lippia javanica (Burm.f.) Spreng. / C. Pretorius Pretorius, Corlea January 2010 (has links) The evolution of aerobic metabolic processes unavoidably led to the production of reactive oxygen species (ROS). ROS have the ability to cause harmful oxidative damage to biomolecules. Increased ROS generation and subsequent oxidative stress have been associated with aging and neurodegenerative disorders such as Parkinson’s and Alzheimer’s diseases as a result of the extreme sensitivity of the central nervous system to damage from ROS. Antioxidant defence systems have co–evolved with aerobic metabolic processes to counteract oxidative damage inflicted by ROS. The impact of neurodegenerative disorders on society is increasing rapidly as the life expectancy of the global population increases. In this day and age, a much younger group of the population is also experiencing neurodegenerative symptoms as a result of the harmful effect of the human immunodeficiency virus (HIV) on the central nervous system. Plants are an invaluable source of medicinal compounds. The use of plants for their healing properties is rooted in ancient times. The aim of this study was to select from twenty one plants, the plant with the most promising antioxidant activity and to determine whether extracts of this plant could act as free radical scavengers, comparing the results to Trolox, a known free radical scavenger. The next step was to isolate and characterize a compound from an extract exhibiting promising antioxidant activity. Bioassay–guided fractionation was followed to achieve this. During screening trials, twenty one plants, namely Berula erecta, Heteromorpha arborescens, Tarchonanthus camphoratus, Vernonia oligocephala, Gymnosporia buxifolia, Acacia karroo, Elephantorrhiza elephantina, Erythrina zeyheri, Leonotis leonurus, Plectranthus ecklonii, P. rehmanii, P. venteri, Salvia auretia, S. runcinata, Solenostemon latifolius, S. rotundifolius, Plumbago auriculata, Clematis brachiata, Vangueria infausta, Physalis peruviana and Lippia javanica were selected from literature, based on reported antioxidant activity within the plant families, for screening of their antioxidant activity. One hundred and ten extracts were prepared from the leaves, using Soxhlet extraction and the solvents petroleum ether (PE), dichloromethane (DCM), ethyl acetate (EtOAc) and ethanol (EtOH), consecutively. The focus during initial screening trials was on chemistry–based assays. The oxygen radical absorbance capacity (ORAC) and ferric reducing antioxidant power (FRAP) assays were employed for the primary screening of the one hundred and ten leaf extracts. The ORAC assay was used to determine whether the plant extracts were able to scavenge peroxyl radicals and the FRAP assay was used to determine the reducing abilities of the extracts. Quantification of the peroxyl radical scavenging activity by the ORAC assay revealed that activity was observed for most of the extracts, with the ethyl acetate and ethanol extracts of L. javanica exhibiting the most promising activity. This pattern of activity was also found with the reducing capacity evaluated by the FRAP assay in which the EtOAc and EtOH extracts of L. javanica also exhibited the most promising activity. L. javanica was selected for further study by screening for biological activity, employing the nitro–blue tetrazolium (NBT) assay and thiobarbituric acid reactive substances (TBARS) assay. Using a cyanide model to induce neurotoxic effects in rat brain homogenate, the neuroprotective properties of the extracts of L. javanica leaves were examined using the NBT assay and compared to that of Trolox. The NBT assay determines the level of superoxide anions. All the extracts of L. javanica significantly reduced superoxide anion generation at all concentrations used. The petroleum ether and ethyl acetate extracts, at all concentrations, reduced superoxide anion generation to values lower than that of the control, suggesting that these extracts may be able to attenuate normal free radical processes in the brain. The petroleum ether extract exhibited the most promising activity at a concentration of 1.25 and 2.5 mg/ml and also exhibited similar results as the ethyl acetate extract at a lower concentration than the ethyl acetate extract (2.5 mg/ml compared to 5 mg/ml). A toxin–solution consisting of hydrogen peroxide (H2O2), iron(III)chloride (FeCl3) and ascorbic acid was used to induce lipid peroxidation and the ability of the extracts of the leaves of L. javanica to attenuate lipid peroxidation was investigated in rat brain homogenate and compared to that of Trolox. All of the extracts of L. javanica significantly attenuated toxininduced lipid peroxidation at all concentrations used. All of the extracts were also able to significantly attenuate toxin–induced lipid peroxidation to values lower than that of the control. These results suggest that all of the extracts of L. javanica possess the ability to attenuate not only toxin–induced lipid peroxidation, but also lipid peroxidation that occurs during normal processes in the brain. The petroleum ether extract was subjected to bioassay–guided fractionation using column and thin–layer chromatography and the NBT and TBARS assays. Fraction DD1 was investigated by means of nuclear magnetic resonance, infrared and mass spectrometry. The exact structure of fraction DD1 was not elucidated. Considering all the results, it is clear that L. javanica shows great potential as a medicinal plant with antioxidant activity and may therefore be beneficial in diminishing the destructive oxidative effects inflicted by free radicals. There are however still many compounds to be isolated from L. javanica. Key words: Verbenaceae, Lippia javanica, antioxidant, neurodegeneration, oxygen radical absorbance capacity (ORAC), ferric reducing antioxidant power (FRAP), nitro–blue tetrazolium assay (NBT), thiobarbituric acid reactive substances assay (TBARS). / Thesis (M.Sc. (Pharmaceutical Chemistry))--North-West University, Potchefstroom Campus, 2011. Verbenaceae Lippia javanica Antioxidant Neurodegeneration Ferric reducing antioxidant power (FRAP) Nitro-blue tetrazolium assay (NBT) Anti-oksidant Neurodegenerasie Nitrobloutetrasolium toets (NBT)

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