AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES

Detalhes bibliográficos
Autor(a) principal: Michel, Renan Garcia
Data de Publicação: 2016
Tipo de documento: Dissertação
Idioma: por
Título da fonte: Biblioteca Digital de Teses e Dissertações do UNICENTRO
Texto Completo: http://tede.unicentro.br:8080/jspui/handle/jspui/690
Resumo: Diabetes mellitus is a disease with high rate of morbi-mortality, that affects millions of people in the whole world, triggering several healthy complications, social and economic repercussions, due to the greatest propensity that diabetic patients have for developing chronic complications, such as heart diseases, nephropathies, neuropathies and retinopathies. In this context, different researches may assist in the search for new alternatives of treatment to improve diabetic patients’ life quality. In the present study a β (1→6) D-Glucan produced by Lasiodiplodia theobromae (MMPI) was utilized to treat diabetes and its symptoms. β-glucans already have well known biological activities, among them, a hypoglycemic one, attributed to β (1→3) D-Glucan, in addition, glucans with β (1→6) bonding are little studied. 30 adult Wistar rats were treated during 28 days. The animals were divided in 5 groups: SC – Saline Control (treated with saline solution); DS – Diabetic Saline (diabetic-induced and treated with saline solution); PC – Positive Control (diabetic-induced treated with metformin); G5 – 5mg of Glucan (diabetic-induced and treated with β(1→6) D-Glucan 5mg/kg of body weight) and G15 - 15mg of Glucan (diabetic-induced and treated with β(1→6) D-Glucan 15mg/kg of body weight). Alloxan was administrated in a concentration of 150 mg/kg of body weight to induce experimental diabetes in the animals. Body weight and fasting capillary blood glucose were weekly analyzed, and OGTT was performed in the 14º day of treatment. In the end of the 28 days’ treatment, euthanasia was made in order to collect biological material to biochemical analyses and quantification of TBARS in renal and hepatic tissues. There was statistical difference (P<0.05) in body weight evolution, capillary blood glucose and oral glucose tolerance test. A decrease of fasting hyperglycemia and also after the administration of glucose was demonstrated, as well as a better body weight evolution of the rats from group G5 and G15 when compared to the DS group. In biochemical parameters, no statistical difference was demonstrated to creatinine and AST (P>0,05). Moreover, there was an enhancement of ALT and urea levels in all diabetic groups. In hepatic biomarkers, there was a rise of total proteins and albumin to DS and G15 groups, respectively (P<0,05). No difference between groups was noticed in liver TBARS dosage (P>0,05), but there was an increase in kidney’s TBARS to all diabetic groups, with a reduction in the values of the groups treated with the glucan (P<0,05). The treatment with β(1→6) D-Glucan was effective in body weight loss control, and reveled a hypoglycemic effect at fasting, allied to an improvement in glucose response. Thus, it was possible to observe an enhancement in total proteins levels and hypoglycemic effect, beyond a discreet protector effect over lipid peroxidation in kidneys.
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spelling MALFATTI, CARLOS RICARDO MANECKhttp://lattes.cnpq.br/7879558601666787SILVA, WEBER CLÁUDIO FRANCISCO NUNES DAhttp://lattes.cnpq.br/1892865713778963065.211.909-38http://lattes.cnpq.br/3482578665906834Michel, Renan Garcia2017-06-12T16:49:59Z2016-09-02Michel, Renan Garcia. AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES. 2016. 60 f. Dissertação (Programa de Pós-Graduação em Ciências Farmacêuticas - Mestrado / Associação Ampla com UEPG) - Universidade Estadual do Centro-Oeste, Guarapuava - PR.http://tede.unicentro.br:8080/jspui/handle/jspui/690Diabetes mellitus is a disease with high rate of morbi-mortality, that affects millions of people in the whole world, triggering several healthy complications, social and economic repercussions, due to the greatest propensity that diabetic patients have for developing chronic complications, such as heart diseases, nephropathies, neuropathies and retinopathies. In this context, different researches may assist in the search for new alternatives of treatment to improve diabetic patients’ life quality. In the present study a β (1→6) D-Glucan produced by Lasiodiplodia theobromae (MMPI) was utilized to treat diabetes and its symptoms. β-glucans already have well known biological activities, among them, a hypoglycemic one, attributed to β (1→3) D-Glucan, in addition, glucans with β (1→6) bonding are little studied. 30 adult Wistar rats were treated during 28 days. The animals were divided in 5 groups: SC – Saline Control (treated with saline solution); DS – Diabetic Saline (diabetic-induced and treated with saline solution); PC – Positive Control (diabetic-induced treated with metformin); G5 – 5mg of Glucan (diabetic-induced and treated with β(1→6) D-Glucan 5mg/kg of body weight) and G15 - 15mg of Glucan (diabetic-induced and treated with β(1→6) D-Glucan 15mg/kg of body weight). Alloxan was administrated in a concentration of 150 mg/kg of body weight to induce experimental diabetes in the animals. Body weight and fasting capillary blood glucose were weekly analyzed, and OGTT was performed in the 14º day of treatment. In the end of the 28 days’ treatment, euthanasia was made in order to collect biological material to biochemical analyses and quantification of TBARS in renal and hepatic tissues. There was statistical difference (P<0.05) in body weight evolution, capillary blood glucose and oral glucose tolerance test. A decrease of fasting hyperglycemia and also after the administration of glucose was demonstrated, as well as a better body weight evolution of the rats from group G5 and G15 when compared to the DS group. In biochemical parameters, no statistical difference was demonstrated to creatinine and AST (P>0,05). Moreover, there was an enhancement of ALT and urea levels in all diabetic groups. In hepatic biomarkers, there was a rise of total proteins and albumin to DS and G15 groups, respectively (P<0,05). No difference between groups was noticed in liver TBARS dosage (P>0,05), but there was an increase in kidney’s TBARS to all diabetic groups, with a reduction in the values of the groups treated with the glucan (P<0,05). The treatment with β(1→6) D-Glucan was effective in body weight loss control, and reveled a hypoglycemic effect at fasting, allied to an improvement in glucose response. Thus, it was possible to observe an enhancement in total proteins levels and hypoglycemic effect, beyond a discreet protector effect over lipid peroxidation in kidneys.O diabetes é uma doença com alta taxa de morbimortalidade, que atinge milhões de pessoas em todo o mundo, trazendo inúmeras complicações à saúde, repercussões sociais e econômicas, isso devido à maior propensão que os pacientes diabéticos têm em desenvolver complicações crônicas, como cardiopatias, nefropatias, neuropatias e retinopatias. Neste contexto, diferentes pesquisas podem auxiliar na busca de novas alternativas de tratamento para a melhoria da qualidade de vida dos diabéticos. Neste trabalho foi utilizada a β (1→6) D-Glucana produzida pelo Lasiodiplodia theobromae (MMPI) para o tratamento do diabetes e seus sintomas. Uma vez que as β-glucanas já possuem atividade biológica conhecida, dentre elas, a hipoglicemiante, atribuida à β (1→3) D-Glucana, além disso, as glucanas com ligação do tipo β (1→6) ainda são pouco estudadas. Foram utilizados 30 ratos adultos da linhagem Wistar tratados durante 28 dias. Os animais foram divididos em 5 grupos: CS – Controle Salinal (tratados com solução salina; DS – Diabético Salina (induzidos ao diabetes e tratados com solução salina; CP – Controle Positivo (induzidos ao diabetes e tratados com Metformina); G5 – Glucana 5mg (induzidos ao diabetes e tratados com β(1→6) D-Glucana 5mg/kg de peso) e G15 - Glucana 15mg (induzidos ao diabetes e tratados com β(1→6) D-Glucana 15mg/kg de peso). Foi administrado aloxana na concentração de 150 mg/kg de peso para o desenvolvimento do diabetes. Os animais foram avaliados semanalmente quanto ao peso e glicemia capilar de jejum, além do TOTG ao 14º dia de tratamento. Ao final dos 28 dias de tratamento os ratos foram eutanasiados para a coleta de material para análises bioquímicas e quantificação de TBARS nos tecidos renais e hepáticos. Houve diferença estatística (P<0,05) na evolução do peso semanal, glicemia capilar e na tolerância oral a glicose, demonstrando diminuição da hiperglicemia de jejum e após carga de glicose, bem como melhor na evolução do peso dos ratos dos grupos G5 e G15 quando comparados ao grupo DS, nos parâmetros bioquímicos, não houve diferença estatística nos valores de creatinina e AST (P>0,05), ainda houve aumento de ALT e ureia em todos os grupos diabéticos, nos marcadores hepáticos ainda houve aumento de proteínas totais e albumina nos grupo DS e G15, respectivamente (P<0,05). Não houve diferença entre os grupos na dosagem de TBARS do fígado (P>0,05), já para o rim houve aumento de TBARS em todos os grupos diabéticos, com redução dos valores nos grupos tratados com glucana (P<0,05). O tratamento com β(1→6) D-Glucana se mostrou eficaz na diminuição da perda de peso, além de um efeito hipoglicemiante de jejum, aliado a melhoria da resposta à glicose. Ainda foi possível observar o aumento dos níveis de proteínas totais e efeito hipotrigliceridêmico, além de um discreto efeito protetor sobre a peroxidação lipídica dos rins.Submitted by Fabiano Jucá (fjuca@unicentro.br) on 2017-06-12T16:49:59Z No. of bitstreams: 1 Renan Garcia Michel.pdf: 2109940 bytes, checksum: cf86e33accd9d7a544ebfa5799ce83f4 (MD5)Made available in DSpace on 2017-06-12T16:49:59Z (GMT). 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dc.title.por.fl_str_mv AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
title AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
spellingShingle AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
Michel, Renan Garcia
Glucana
Diabetes
Lasiodiplodia theobromae
Exopolisscarídeo
Glucan
Diabetes
Lasiodiplodia theobromae
Exopolysaccharides
CIENCIAS DA SAUDE::FARMACIA
title_short AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
title_full AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
title_fullStr AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
title_full_unstemmed AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
title_sort AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES
author Michel, Renan Garcia
author_facet Michel, Renan Garcia
author_role author
dc.contributor.advisor1.fl_str_mv MALFATTI, CARLOS RICARDO MANECK
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/7879558601666787
dc.contributor.advisor-co1.fl_str_mv SILVA, WEBER CLÁUDIO FRANCISCO NUNES DA
dc.contributor.advisor-co1Lattes.fl_str_mv http://lattes.cnpq.br/1892865713778963
dc.contributor.authorID.fl_str_mv 065.211.909-38
dc.contributor.authorLattes.fl_str_mv http://lattes.cnpq.br/3482578665906834
dc.contributor.author.fl_str_mv Michel, Renan Garcia
contributor_str_mv MALFATTI, CARLOS RICARDO MANECK
SILVA, WEBER CLÁUDIO FRANCISCO NUNES DA
dc.subject.por.fl_str_mv Glucana
Diabetes
Lasiodiplodia theobromae
Exopolisscarídeo
topic Glucana
Diabetes
Lasiodiplodia theobromae
Exopolisscarídeo
Glucan
Diabetes
Lasiodiplodia theobromae
Exopolysaccharides
CIENCIAS DA SAUDE::FARMACIA
dc.subject.eng.fl_str_mv Glucan
Diabetes
Lasiodiplodia theobromae
Exopolysaccharides
dc.subject.cnpq.fl_str_mv CIENCIAS DA SAUDE::FARMACIA
description Diabetes mellitus is a disease with high rate of morbi-mortality, that affects millions of people in the whole world, triggering several healthy complications, social and economic repercussions, due to the greatest propensity that diabetic patients have for developing chronic complications, such as heart diseases, nephropathies, neuropathies and retinopathies. In this context, different researches may assist in the search for new alternatives of treatment to improve diabetic patients’ life quality. In the present study a β (1→6) D-Glucan produced by Lasiodiplodia theobromae (MMPI) was utilized to treat diabetes and its symptoms. β-glucans already have well known biological activities, among them, a hypoglycemic one, attributed to β (1→3) D-Glucan, in addition, glucans with β (1→6) bonding are little studied. 30 adult Wistar rats were treated during 28 days. The animals were divided in 5 groups: SC – Saline Control (treated with saline solution); DS – Diabetic Saline (diabetic-induced and treated with saline solution); PC – Positive Control (diabetic-induced treated with metformin); G5 – 5mg of Glucan (diabetic-induced and treated with β(1→6) D-Glucan 5mg/kg of body weight) and G15 - 15mg of Glucan (diabetic-induced and treated with β(1→6) D-Glucan 15mg/kg of body weight). Alloxan was administrated in a concentration of 150 mg/kg of body weight to induce experimental diabetes in the animals. Body weight and fasting capillary blood glucose were weekly analyzed, and OGTT was performed in the 14º day of treatment. In the end of the 28 days’ treatment, euthanasia was made in order to collect biological material to biochemical analyses and quantification of TBARS in renal and hepatic tissues. There was statistical difference (P<0.05) in body weight evolution, capillary blood glucose and oral glucose tolerance test. A decrease of fasting hyperglycemia and also after the administration of glucose was demonstrated, as well as a better body weight evolution of the rats from group G5 and G15 when compared to the DS group. In biochemical parameters, no statistical difference was demonstrated to creatinine and AST (P>0,05). Moreover, there was an enhancement of ALT and urea levels in all diabetic groups. In hepatic biomarkers, there was a rise of total proteins and albumin to DS and G15 groups, respectively (P<0,05). No difference between groups was noticed in liver TBARS dosage (P>0,05), but there was an increase in kidney’s TBARS to all diabetic groups, with a reduction in the values of the groups treated with the glucan (P<0,05). The treatment with β(1→6) D-Glucan was effective in body weight loss control, and reveled a hypoglycemic effect at fasting, allied to an improvement in glucose response. Thus, it was possible to observe an enhancement in total proteins levels and hypoglycemic effect, beyond a discreet protector effect over lipid peroxidation in kidneys.
publishDate 2016
dc.date.issued.fl_str_mv 2016-09-02
dc.date.accessioned.fl_str_mv 2017-06-12T16:49:59Z
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dc.identifier.citation.fl_str_mv Michel, Renan Garcia. AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES. 2016. 60 f. Dissertação (Programa de Pós-Graduação em Ciências Farmacêuticas - Mestrado / Associação Ampla com UEPG) - Universidade Estadual do Centro-Oeste, Guarapuava - PR.
dc.identifier.uri.fl_str_mv http://tede.unicentro.br:8080/jspui/handle/jspui/690
identifier_str_mv Michel, Renan Garcia. AVALIAÇÃO DO EFEITO DA Β (1→6) D-GLUCANA PRODUZIDA PELO FUNGO LASIODIPLODIA THEOBROMAE MMPI SOBRE UM MODELO ANIMAL DE DIABETES. 2016. 60 f. Dissertação (Programa de Pós-Graduação em Ciências Farmacêuticas - Mestrado / Associação Ampla com UEPG) - Universidade Estadual do Centro-Oeste, Guarapuava - PR.
url http://tede.unicentro.br:8080/jspui/handle/jspui/690
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