Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental

Detalhes bibliográficos
Ano de defesa: 2016
Autor(a) principal: Nogueira, Guilherme Baia [UNIFESP]
Orientador(a): Não Informado pela instituição
Banca de defesa: Não Informado pela instituição
Tipo de documento: Dissertação
Tipo de acesso: Acesso aberto
dARK ID: ark:/48912/001300001ks49
Idioma: por
Instituição de defesa: Universidade Federal de São Paulo (UNIFESP)
Programa de Pós-Graduação: Não Informado pela instituição
Departamento: Não Informado pela instituição
País: Não Informado pela instituição
Palavras-chave em Português:
N-acetylcysteine
Antioxidant
Nitric oxide
Experimental diabetes mellitus
Diabetic nephropathy and oxidative stress
N-acetilcisteína
Antioxidante
Óxido nítrico
Diabetes mellitus experimental
Nefropatia diabética e estresse oxidativo
Link de acesso: https://sucupira.capes.gov.br/sucupira/public/consultas/coleta/trabalhoConclusao/viewTrabalhoConclusao.jsf?popup=true&id_trabalho=4699339
http://repositorio.unifesp.br/handle/11600/47341
Resumo: INTRODUCTION : Diabetes mellitus (DM) induces intra and extracellular changes, with substantial increase in reactive oxygen species (ROS). ROS causes damage to the systemic and renal microvasculature, which could be one of the mechanisms involved in the development of diabetic nephropathy. ROS modulate other substances like the nitric oxide (NO), a powerful vasodilator with important role in the kidney function. N-acetylcysteine (NAC) is an antioxidant that acts replenishing intracellular cysteine levels, which is essencial in the glutathione (GSH) formation. OBJECTIVE : The aim of this study was to evaluate the effect of early or late treatment with N-acetylcysteine on oxidative/nitrosative stress control in experimental diabetic nephropathy. MATERIAL AND METHODS: We used 60 adult male Wistar rats that underwent unilateral nephrectomy. Diabetes was induced with streptozotocin (60 mg / kg, iv) in 40 animals (DM) and the others received vehicle (CTL). Half of CTL animals were supplemented with NAC (600mg/L of water, ad libitum, CTL+NAC) and the others received water as NAC vehicle. 10 diabetic animals received NAC [600mg/L of water, ad libitum, DM+NAC (PRE)] and 10 received the NAC vehicle [water, DM (PRE)] during 8 weeks after diabetes induction. 10 animals received NAC [600mg/L of water, ad libitum, DM+NAC (TAR)] and 10 received the NAC vehicle [water, DM (TAR)] for 8 weeks, beginning after 4 weeks of diabetes. N = 10 each group. Before any procedure and before and after the early or late treatment protocol with NAC, we collected urine and blood and only at the end of the protocol, the kidney tissue was removed for further analysis. Data were expressed as mean±SEM and analyzed by non-parametric statistical analysis and unpaired t test or one-way ANOVA with Tukey's post-test, when appropriate; it was considered statistically significant when p<0.05. RESULTS : DM (PRE) compared to CTL showed a significant increase in glycemia levels (mg/dL): 509.0±19.6 vs 85.0±3.7, impaired renal function with increased plasmatic creatinine (mg/dL): 2.0± 0.1 vs 1.1±0.1 and urea (mg/dL): 92.3± 8.3 vs 51.9±5.2 and proteinuria (mg/24h): 40.1±3.9 vs 17.7±2.9 and also a reduction in creatinine clearance (mL/min): 1.0±0.1 vs 1.8±0.1. DM (PRE) vs CTL showed a significant increase in TBARS, a lipoperoxidation marker in plasma (nmol/mL), urine (nmol/24h) and kidney tissue (nmol/mg of protein): 5.0±0.7 vs 2.9±0.1; 446.7±19.2 vs 97.7±8.5 and 8.0±0.8 vs 5.3±0.5, respectively, and also a significant decrease in plasmatic NO (mM): 35.4±2.1 vs 54.4±3.8. Analysis of these two groups by means of western blotting showed that DM group (PRE) increased iNOS (0.8±0.2 vs 0.3±0.1) and decreased eNOS (0.9±0.1 vs 1.6±0.2), both p<0.05. Early NAC supplementation in DM rats reduced proteinuria (18.2±2.3), plasmatic creatinine (1.5±0.1) and urea (66.1±2.3) and a decrease in TBARS levels, in plasma, urine and renal tissue (2.6±0.1, 326.0±5.7 and 35.9±0.3), as well as increased creatinine clearance (1.9±0.4), plasma NO (59.8±5.2) and eNOS (1.3±0.1), and reduction of iNOS (0.4±0.1) vs DM (PRE), all p<0.05. This early treatment in DM rats significantly increased antioxidant defenses promoting increased catalase (1.3±0.1 vs 0.7±0.1) and glutathione (1.4±0.1 vs 0.9±0.1). In late treatment with NAC in DM rats as compared to DM rats without NAC, we found decreased proteinuria (32.6±6.0 vs 61.6±7.9) and TBARS excretion (284.8±26.0 vs 326.0±35.9) and increased creatinine clearance (1.4±0.1 vs 0.7±0.1) and NO plasmatic (60.1±3.4 vs 41.4±2.3), all statistically significant. Histological analysis of the diabetic rats without treatment with NAC, [DM (PRE) or DM (TAR)] showed significant tubular changes with degeneration and vacuolization in tubular cells, dilated tubular lumen, intense glycosidic degeneration, and discrete mesangial expansion with interstitial fibrosis area. DM + NAC (PRE) also showed intense glycosidic degeneration, but did not present tubular degeneration or fibrosis. DM+NAC (TAR) showed severe glycosidic degeneration, moderate tubular cell degeneration, light and focal dilatation of the tubules, without fibrosis. CONCLUSION : Our study showed that NAC protected the diabetic rats against renal injury, probably due to the control of oxidative stress and/or increased NO bioavailability, showing that early NAC was more effective than late treatment. This suggests that NAC may be useful in the adjuvant treatment of diabetic patients in the early phase of the disease. Eventually, prolonged treatment, even if it is started later, could change the natural history of the disease, improving survival and quality of life in diabetic patients.
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spelling Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimentalEvaluation of early or late N­-acetylcysteine treatment on the oxidative/nitrosative stress control in experimental diabetic nephropathyN-acetylcysteineAntioxidantNitric oxideExperimental diabetes mellitusDiabetic nephropathy and oxidative stressN-acetilcisteínaAntioxidanteÓxido nítricoDiabetes mellitus experimentalNefropatia diabética e estresse oxidativoINTRODUCTION : Diabetes mellitus (DM) induces intra and extracellular changes, with substantial increase in reactive oxygen species (ROS). ROS causes damage to the systemic and renal microvasculature, which could be one of the mechanisms involved in the development of diabetic nephropathy. ROS modulate other substances like the nitric oxide (NO), a powerful vasodilator with important role in the kidney function. N-acetylcysteine (NAC) is an antioxidant that acts replenishing intracellular cysteine levels, which is essencial in the glutathione (GSH) formation. OBJECTIVE : The aim of this study was to evaluate the effect of early or late treatment with N-acetylcysteine on oxidative/nitrosative stress control in experimental diabetic nephropathy. MATERIAL AND METHODS: We used 60 adult male Wistar rats that underwent unilateral nephrectomy. Diabetes was induced with streptozotocin (60 mg / kg, iv) in 40 animals (DM) and the others received vehicle (CTL). Half of CTL animals were supplemented with NAC (600mg/L of water, ad libitum, CTL+NAC) and the others received water as NAC vehicle. 10 diabetic animals received NAC [600mg/L of water, ad libitum, DM+NAC (PRE)] and 10 received the NAC vehicle [water, DM (PRE)] during 8 weeks after diabetes induction. 10 animals received NAC [600mg/L of water, ad libitum, DM+NAC (TAR)] and 10 received the NAC vehicle [water, DM (TAR)] for 8 weeks, beginning after 4 weeks of diabetes. N = 10 each group. Before any procedure and before and after the early or late treatment protocol with NAC, we collected urine and blood and only at the end of the protocol, the kidney tissue was removed for further analysis. Data were expressed as mean±SEM and analyzed by non-parametric statistical analysis and unpaired t test or one-way ANOVA with Tukey's post-test, when appropriate; it was considered statistically significant when p<0.05. RESULTS : DM (PRE) compared to CTL showed a significant increase in glycemia levels (mg/dL): 509.0±19.6 vs 85.0±3.7, impaired renal function with increased plasmatic creatinine (mg/dL): 2.0± 0.1 vs 1.1±0.1 and urea (mg/dL): 92.3± 8.3 vs 51.9±5.2 and proteinuria (mg/24h): 40.1±3.9 vs 17.7±2.9 and also a reduction in creatinine clearance (mL/min): 1.0±0.1 vs 1.8±0.1. DM (PRE) vs CTL showed a significant increase in TBARS, a lipoperoxidation marker in plasma (nmol/mL), urine (nmol/24h) and kidney tissue (nmol/mg of protein): 5.0±0.7 vs 2.9±0.1; 446.7±19.2 vs 97.7±8.5 and 8.0±0.8 vs 5.3±0.5, respectively, and also a significant decrease in plasmatic NO (mM): 35.4±2.1 vs 54.4±3.8. Analysis of these two groups by means of western blotting showed that DM group (PRE) increased iNOS (0.8±0.2 vs 0.3±0.1) and decreased eNOS (0.9±0.1 vs 1.6±0.2), both p<0.05. Early NAC supplementation in DM rats reduced proteinuria (18.2±2.3), plasmatic creatinine (1.5±0.1) and urea (66.1±2.3) and a decrease in TBARS levels, in plasma, urine and renal tissue (2.6±0.1, 326.0±5.7 and 35.9±0.3), as well as increased creatinine clearance (1.9±0.4), plasma NO (59.8±5.2) and eNOS (1.3±0.1), and reduction of iNOS (0.4±0.1) vs DM (PRE), all p<0.05. This early treatment in DM rats significantly increased antioxidant defenses promoting increased catalase (1.3±0.1 vs 0.7±0.1) and glutathione (1.4±0.1 vs 0.9±0.1). In late treatment with NAC in DM rats as compared to DM rats without NAC, we found decreased proteinuria (32.6±6.0 vs 61.6±7.9) and TBARS excretion (284.8±26.0 vs 326.0±35.9) and increased creatinine clearance (1.4±0.1 vs 0.7±0.1) and NO plasmatic (60.1±3.4 vs 41.4±2.3), all statistically significant. Histological analysis of the diabetic rats without treatment with NAC, [DM (PRE) or DM (TAR)] showed significant tubular changes with degeneration and vacuolization in tubular cells, dilated tubular lumen, intense glycosidic degeneration, and discrete mesangial expansion with interstitial fibrosis area. DM + NAC (PRE) also showed intense glycosidic degeneration, but did not present tubular degeneration or fibrosis. DM+NAC (TAR) showed severe glycosidic degeneration, moderate tubular cell degeneration, light and focal dilatation of the tubules, without fibrosis. CONCLUSION : Our study showed that NAC protected the diabetic rats against renal injury, probably due to the control of oxidative stress and/or increased NO bioavailability, showing that early NAC was more effective than late treatment. This suggests that NAC may be useful in the adjuvant treatment of diabetic patients in the early phase of the disease. Eventually, prolonged treatment, even if it is started later, could change the natural history of the disease, improving survival and quality of life in diabetic patients.Introdução Diabetes mellitus (DM) induz a mudanças intra e extracelulares, com aumento substancial de espécies reativas de oxigênio (ROS). ROS causam danos na microvasculatura sistêmica e renal, o que poderia ser um dos mecanismos envolvidos na fisiopatologia da nefropatia diabética. As ROS modulam substâncias como o óxido nítrico (NO), potente vasodilatador com papel importante na função renal. A N-acetilcisteína (NAC) é um antioxidante que atua reabastecendo os níveis intracelulares de cisteína, importante na formação da glutationa (GSH). Objetivo O objetivo deste estudo foi avaliar o efeito do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo/nitrosativo na nefropatia diabética experimental. MATERIAL E Métodos Utilizamos 60 ratos machos Wistar adultos que foram submetidos à nefrectomia unilateral. O diabetes foi induzido com estreptozotocina (60mg/kg, iv) em 40 animais (DM) e os demais receberam o seu veículo (CTL). Metade dos animais CTL receberam suplementação com NAC (600mg/L de água, ad libitum, CTL+NAC) e os demais receberam água como veículo da NAC. 10 animais diabéticos receberam NAC [600mg/L de água, ad libitum, DM+NAC (PRE)] e 10 receberam o veículo da NAC [água, DM (PRE)] durante 8 semanas após indução do diabetes. 10 animais receberam NAC [600mg/L de água, ad libitum, DM+NAC (TAR)] e 10 receberam o veículo da NAC [água, DM (TAR)] durante 8 semanas, iniciado após a 4ª semana de diabetes. N=10 cada grupo. Antes de qualquer manipulação dos animais, antes e depois dos tratamentos precoce ou tardio com NAC durante oito semanas, foram coletados urina e sangue e no final do protocolo, o tecido renal. Os dados foram expressos como média±EP e analisados através da análise estatística não paramétrica e não pareada t test, ou do teste one-way ANOVA, com o pós-teste de Tukey, quando apropriados, sendo considerados estatisticamente significantes quando p<0,05. xix Resultados DM (PRE) comparado com CTL mostrou aumento significante dos níveis de glicemia (mg/dL): 509,0±19,6 vs 85,0±3,7 e apresentou função renal alterada, com aumento da creatinina (mg/dL): 2,0±0,1 vs 1,1±0,1 e ureia plasmáticas (mg/dL): 92,3±8,3 vs 51,9±5,2 e da proteinúria (mg/24h): 40,1±3,9 vs 17,7±2,9 e ainda, redução do clearance de creatinina (mL/min): 1,0±0,1 vs 1,8±0,1. DM (PRE) apresentou aumento significante do TBARS, marcador de lipoperoxidação, no plasma (nmol/mL), urina (nmol/24h) e tecido renal (nmol/mg de proteína), respectivamente: 5,0±0,7 vs 2,9±0,1; 446,7±19,2 vs 97,7±8,5 e 8,0±0,8 vs 5,3±0,5 e também diminuição significante do NO plasmático (?M): 35,4±2,1 vs 54,4±3,8. A análise por meio do western blotting do grupo DM (PRE) mostrou aumento da enzima iNOS (0,8±0,2 vs 0,3±0,1) e diminuição da eNOS (0,9±0,1 vs 1,6±0,2), ambos p<0,05. A suplementação precoce de NAC em ratos DM reduziu a proteinúria (18,2±2,3), creatinina (1,5±0,1) e ureia plasmáticas (66,1±2,3) e atenuou os níveis de TBARS, no plasma, urina e tecido renal (2,6±0,1; 326,0±35,9 e 5,7±0,3), bem como causou aumento do clearance de creatinina (1,9±0,4), NO plasmático (59,8±5,2) e da eNOS (1,3±0,1), além da diminuição da iNOS (0,4±0,1), todos p<0,05. Esse tratamento precoce nos ratos DM também aumentou significantemente as defesas antioxidantes promovendo aumento da catalase (1,3±0,1 vs 0,7±0,1) e da glutationa (1,4±0,1 vs 0,9±0,1). No tratamento tardio com NAC em ratos DM, verificamos diminuição da proteinúria (32,6±6,0 vs 61,6±7,9) e da excreção de TBARS (284,8±26,0 vs 326,0±35,9) e aumento do clearance de creatinina (1,4±0,1 vs 0,7±0,1) e do NO plasmático (60,1±3,4 vs 41,4±2,3), sendo todos estatisticamente significantes. A análise histológica dos ratos diabéticos sem tratamento com NAC [DM(PRE) ou DM (TAR)] mostrou alterações tubulares importantes, tendo como as principais, degeneração das células tubulares, luz tubular dilatada, intensa degeneração glicosídica, além de expansão mesangial e discreta área de fibrose intersticial. Os animais do grupo DM+NAC (PRE) apresentaram também intensa degeneração glicosídica, entretanto não mostraram degeneração tubular e fibrose. Os animais que receberam NAC tardiamente mostraram intensa degeneração glicosídica, moderada degeneração das células tubulares para a luz e dilatação focal dos túbulos e não apresentavam fibrose. Conclusão xx O nosso estudo em ratos diabéticos evidenciou que a NAC protegeu contra a lesão renal, provavelmente devido ao controle do estresse oxidativo e / ou aumento da biodisponibilidade de NO, revelando que o tratamento precoce foi mais eficaz que o tardio, sugerindo que a NAC pode ser útil no tratamento coadjuvante de pacientes diabéticos no início da doença. Eventualmente o tratamento prolongado, mesmo que seja iniciado mais tarde, altere a história natural da doença, melhorando a sobrevida e a qualidade de vida de pacientes diabéticos.Dados abertos - Sucupira - Teses e dissertações (2013 a 2016)Universidade Federal de São Paulo (UNIFESP)Higa, Elisa Mieko Suemitsu [UNIFESP]http://lattes.cnpq.br/8578252701813423http://lattes.cnpq.br/7424286665954116Universidade Federal de São Paulo (UNIFESP)Nogueira, Guilherme Baia [UNIFESP]2018-07-30T11:44:21Z2018-07-30T11:44:21Z2016-06-30info:eu-repo/semantics/masterThesisinfo:eu-repo/semantics/publishedVersionapplication/pdfhttps://sucupira.capes.gov.br/sucupira/public/consultas/coleta/trabalhoConclusao/viewTrabalhoConclusao.jsf?popup=true&id_trabalho=4699339NOGUEIRA, Guilherme Baia. Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental. 2016. Dissertação (Mestrado em Medicina: Nefrologia) - Escola Paulista de Medicina, Universidade Federal de São Paulo (UNIFESP), São Paulo, 2016.2016-0628.pdfhttp://repositorio.unifesp.br/handle/11600/47341ark:/48912/001300001ks49porSão Pauloinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UNIFESPinstname:Universidade Federal de São Paulo (UNIFESP)instacron:UNIFESP2024-08-01T15:57:00Zoai:repositorio.unifesp.br:11600/47341Repositório InstitucionalPUBhttp://www.repositorio.unifesp.br/oai/requestbiblioteca.csp@unifesp.bropendoar:34652024-08-01T15:57Repositório Institucional da UNIFESP - Universidade Federal de São Paulo (UNIFESP)false
dc.title.none.fl_str_mv Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
Evaluation of early or late N­-acetylcysteine treatment on the oxidative/nitrosative stress control in experimental diabetic nephropathy
title Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
spellingShingle Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
Nogueira, Guilherme Baia [UNIFESP]
N-acetylcysteine
Antioxidant
Nitric oxide
Experimental diabetes mellitus
Diabetic nephropathy and oxidative stress
N-acetilcisteína
Antioxidante
Óxido nítrico
Diabetes mellitus experimental
Nefropatia diabética e estresse oxidativo
title_short Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
title_full Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
title_fullStr Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
title_full_unstemmed Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
title_sort Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental
author Nogueira, Guilherme Baia [UNIFESP]
author_facet Nogueira, Guilherme Baia [UNIFESP]
author_role author
dc.contributor.none.fl_str_mv Higa, Elisa Mieko Suemitsu [UNIFESP]
http://lattes.cnpq.br/8578252701813423
http://lattes.cnpq.br/7424286665954116
Universidade Federal de São Paulo (UNIFESP)
dc.contributor.author.fl_str_mv Nogueira, Guilherme Baia [UNIFESP]
dc.subject.por.fl_str_mv N-acetylcysteine
Antioxidant
Nitric oxide
Experimental diabetes mellitus
Diabetic nephropathy and oxidative stress
N-acetilcisteína
Antioxidante
Óxido nítrico
Diabetes mellitus experimental
Nefropatia diabética e estresse oxidativo
topic N-acetylcysteine
Antioxidant
Nitric oxide
Experimental diabetes mellitus
Diabetic nephropathy and oxidative stress
N-acetilcisteína
Antioxidante
Óxido nítrico
Diabetes mellitus experimental
Nefropatia diabética e estresse oxidativo
description INTRODUCTION : Diabetes mellitus (DM) induces intra and extracellular changes, with substantial increase in reactive oxygen species (ROS). ROS causes damage to the systemic and renal microvasculature, which could be one of the mechanisms involved in the development of diabetic nephropathy. ROS modulate other substances like the nitric oxide (NO), a powerful vasodilator with important role in the kidney function. N-acetylcysteine (NAC) is an antioxidant that acts replenishing intracellular cysteine levels, which is essencial in the glutathione (GSH) formation. OBJECTIVE : The aim of this study was to evaluate the effect of early or late treatment with N-acetylcysteine on oxidative/nitrosative stress control in experimental diabetic nephropathy. MATERIAL AND METHODS: We used 60 adult male Wistar rats that underwent unilateral nephrectomy. Diabetes was induced with streptozotocin (60 mg / kg, iv) in 40 animals (DM) and the others received vehicle (CTL). Half of CTL animals were supplemented with NAC (600mg/L of water, ad libitum, CTL+NAC) and the others received water as NAC vehicle. 10 diabetic animals received NAC [600mg/L of water, ad libitum, DM+NAC (PRE)] and 10 received the NAC vehicle [water, DM (PRE)] during 8 weeks after diabetes induction. 10 animals received NAC [600mg/L of water, ad libitum, DM+NAC (TAR)] and 10 received the NAC vehicle [water, DM (TAR)] for 8 weeks, beginning after 4 weeks of diabetes. N = 10 each group. Before any procedure and before and after the early or late treatment protocol with NAC, we collected urine and blood and only at the end of the protocol, the kidney tissue was removed for further analysis. Data were expressed as mean±SEM and analyzed by non-parametric statistical analysis and unpaired t test or one-way ANOVA with Tukey's post-test, when appropriate; it was considered statistically significant when p<0.05. RESULTS : DM (PRE) compared to CTL showed a significant increase in glycemia levels (mg/dL): 509.0±19.6 vs 85.0±3.7, impaired renal function with increased plasmatic creatinine (mg/dL): 2.0± 0.1 vs 1.1±0.1 and urea (mg/dL): 92.3± 8.3 vs 51.9±5.2 and proteinuria (mg/24h): 40.1±3.9 vs 17.7±2.9 and also a reduction in creatinine clearance (mL/min): 1.0±0.1 vs 1.8±0.1. DM (PRE) vs CTL showed a significant increase in TBARS, a lipoperoxidation marker in plasma (nmol/mL), urine (nmol/24h) and kidney tissue (nmol/mg of protein): 5.0±0.7 vs 2.9±0.1; 446.7±19.2 vs 97.7±8.5 and 8.0±0.8 vs 5.3±0.5, respectively, and also a significant decrease in plasmatic NO (mM): 35.4±2.1 vs 54.4±3.8. Analysis of these two groups by means of western blotting showed that DM group (PRE) increased iNOS (0.8±0.2 vs 0.3±0.1) and decreased eNOS (0.9±0.1 vs 1.6±0.2), both p<0.05. Early NAC supplementation in DM rats reduced proteinuria (18.2±2.3), plasmatic creatinine (1.5±0.1) and urea (66.1±2.3) and a decrease in TBARS levels, in plasma, urine and renal tissue (2.6±0.1, 326.0±5.7 and 35.9±0.3), as well as increased creatinine clearance (1.9±0.4), plasma NO (59.8±5.2) and eNOS (1.3±0.1), and reduction of iNOS (0.4±0.1) vs DM (PRE), all p<0.05. This early treatment in DM rats significantly increased antioxidant defenses promoting increased catalase (1.3±0.1 vs 0.7±0.1) and glutathione (1.4±0.1 vs 0.9±0.1). In late treatment with NAC in DM rats as compared to DM rats without NAC, we found decreased proteinuria (32.6±6.0 vs 61.6±7.9) and TBARS excretion (284.8±26.0 vs 326.0±35.9) and increased creatinine clearance (1.4±0.1 vs 0.7±0.1) and NO plasmatic (60.1±3.4 vs 41.4±2.3), all statistically significant. Histological analysis of the diabetic rats without treatment with NAC, [DM (PRE) or DM (TAR)] showed significant tubular changes with degeneration and vacuolization in tubular cells, dilated tubular lumen, intense glycosidic degeneration, and discrete mesangial expansion with interstitial fibrosis area. DM + NAC (PRE) also showed intense glycosidic degeneration, but did not present tubular degeneration or fibrosis. DM+NAC (TAR) showed severe glycosidic degeneration, moderate tubular cell degeneration, light and focal dilatation of the tubules, without fibrosis. CONCLUSION : Our study showed that NAC protected the diabetic rats against renal injury, probably due to the control of oxidative stress and/or increased NO bioavailability, showing that early NAC was more effective than late treatment. This suggests that NAC may be useful in the adjuvant treatment of diabetic patients in the early phase of the disease. Eventually, prolonged treatment, even if it is started later, could change the natural history of the disease, improving survival and quality of life in diabetic patients.
publishDate 2016
dc.date.none.fl_str_mv 2016-06-30
2018-07-30T11:44:21Z
2018-07-30T11:44:21Z
dc.type.driver.fl_str_mv info:eu-repo/semantics/masterThesis
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
format masterThesis
status_str publishedVersion
dc.identifier.uri.fl_str_mv https://sucupira.capes.gov.br/sucupira/public/consultas/coleta/trabalhoConclusao/viewTrabalhoConclusao.jsf?popup=true&id_trabalho=4699339
NOGUEIRA, Guilherme Baia. Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental. 2016. Dissertação (Mestrado em Medicina: Nefrologia) - Escola Paulista de Medicina, Universidade Federal de São Paulo (UNIFESP), São Paulo, 2016.
2016-0628.pdf
http://repositorio.unifesp.br/handle/11600/47341
dc.identifier.dark.fl_str_mv ark:/48912/001300001ks49
url https://sucupira.capes.gov.br/sucupira/public/consultas/coleta/trabalhoConclusao/viewTrabalhoConclusao.jsf?popup=true&id_trabalho=4699339
http://repositorio.unifesp.br/handle/11600/47341
identifier_str_mv NOGUEIRA, Guilherme Baia. Avaliação do tratamento precoce ou tardio com N-acetilcisteína sobre o controle do estresse oxidativo na nefropatia diabética experimental. 2016. Dissertação (Mestrado em Medicina: Nefrologia) - Escola Paulista de Medicina, Universidade Federal de São Paulo (UNIFESP), São Paulo, 2016.
2016-0628.pdf
ark:/48912/001300001ks49
dc.language.iso.fl_str_mv por
language por
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.coverage.none.fl_str_mv São Paulo
dc.publisher.none.fl_str_mv Universidade Federal de São Paulo (UNIFESP)
publisher.none.fl_str_mv Universidade Federal de São Paulo (UNIFESP)
dc.source.none.fl_str_mv reponame:Repositório Institucional da UNIFESP
instname:Universidade Federal de São Paulo (UNIFESP)
instacron:UNIFESP
instname_str Universidade Federal de São Paulo (UNIFESP)
instacron_str UNIFESP
institution UNIFESP
reponame_str Repositório Institucional da UNIFESP
collection Repositório Institucional da UNIFESP
repository.name.fl_str_mv Repositório Institucional da UNIFESP - Universidade Federal de São Paulo (UNIFESP)
repository.mail.fl_str_mv biblioteca.csp@unifesp.br
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