Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente

Detalhes bibliográficos
Ano de defesa: 2012
Autor(a) principal: Neves, Julliana Catharina de Sousa
Orientador(a): Andrade, Geanne Matos de
Banca de defesa: Não Informado pela instituição
Tipo de documento: Dissertação
Tipo de acesso: Acesso aberto
Idioma: por
Instituição de defesa: Não Informado pela instituição
Programa de Pós-Graduação: Não Informado pela instituição
Departamento: Não Informado pela instituição
País: Não Informado pela instituição
Palavras-chave em Português:
Berberina
Isquemia Encefálica
Estresse Oxidativo
Link de acesso: http://www.repositorio.ufc.br/handle/riufc/4709
Resumo: Stroke is the second leading cause death in industrialized countries and can be subdivided into 2 categories, ischemic and hemorrhagic. The mechanisms of ischemic brain damage involve oxidative stress, excitotoxicity, mitochondrial dysfunction, inflammation and apoptosis. Berberine (BE) is an alkaloid derived from Coptidis rhizom which has potent anti-inflammatory and anti-apoptotic effects. In present study, the neuroprotector effect of berberine after permanent middle cerebral artery occlusion (MCAO) was investigated. Male Swiss mice were divided into five groups (n=8): Sham operated (SO), MCAO, BE 50 and 100mg/kg/day plus MCAO. BE or vehicle (distilled water) were administrated intragastrically 30 min before MCAO (induced by electrocoagulation) and daily during 3 days. The parameters studied were sensorimotor function, working, object recognition, spatial and aversive memory, cerebral infarct area, myeloperoxidase (MPO) and reduced glutathione (GSH) levels and neurodegeneration through FluoroJade C staining. After MCAO a significant decrease of motor performance and sensory function was found after a neurological evaluation. However, berberine did not improve this neurological deficit. Ischemia caused a 70% increase of infarct area in MCAO group compared with SO, that was decreased by treatment with BE 50 and 100. We observed an increase of vertical exploratory activity (rearings) in the BE 100 group compared to the MCAO. BE 100 treatment also improved MCAO-induced late memory deficits in passive avoidance test (latency - SO: 235.0 ± 33.3s; MCAO: 84.7 ± 23.3s; MCAO + BE100: 300.0 ± 0.0s, p<0.05) and MCAO-induced spatial memory deficits evaluated by water maze test (latency - SO: 10.8 ± 2.4%; MCAO: 23.4 ± 3.9%; MCAO + BE100: 12.8 ± 2.0; p<0.05). BE 50 and 100 treatment significantly prevented the MCAO-induced working memory deficits in y-maze test (spontaneous alternations - SO: 73.8 ± 1.9%; MCAO: 57.2 ± 2.7%; MCAO + BE50: 69.3 ± 3.5; MCAO + BE100: 71.9 ± 3.97%; p<0.05) and object recognition memory deficits (recognition index - SO: 0.51 ± 0.09%; MCAO: 0.068 ± 0.12%; MCAO + BE50: 0.42 ± 0.09%; MCAO + BE100: 0.58 ± 0.16%; p<0.05, Kruskall-Wallis, Mann-Whitney). Neuronal degeneration on berberine-treated groups was significantly less than those submitted to MCAO. Mice submitted to MCAO showed an increase in GSH and MPO levels. BE 100 treatment prevented the increase in MPO activity on striatum (SO: 1.53 ± 0.48; MCAO: 4.89 ± 0.89; MCAO + BE100: 2.52 ± 0.47; p<0.05, ANOVA, Newman-Keuls). Berberine showed a significant protective effect against cerebral ischemia, at least by an anti-inflammatory effect.
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spelling Neves, Julliana Catharina de SousaAndrade, Geanne Matos de2013-03-15T12:32:48Z2013-03-15T12:32:48Z2012NEVES, J. C. S. Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente. 2012. 98 f. Dissertação (Mestrado em Farmacologia) - Faculdade de Farmácia, Odontologia e Enfermagem, Universidade Federal do Ceará, Fortaleza, 2012.http://www.repositorio.ufc.br/handle/riufc/4709Stroke is the second leading cause death in industrialized countries and can be subdivided into 2 categories, ischemic and hemorrhagic. The mechanisms of ischemic brain damage involve oxidative stress, excitotoxicity, mitochondrial dysfunction, inflammation and apoptosis. Berberine (BE) is an alkaloid derived from Coptidis rhizom which has potent anti-inflammatory and anti-apoptotic effects. In present study, the neuroprotector effect of berberine after permanent middle cerebral artery occlusion (MCAO) was investigated. Male Swiss mice were divided into five groups (n=8): Sham operated (SO), MCAO, BE 50 and 100mg/kg/day plus MCAO. BE or vehicle (distilled water) were administrated intragastrically 30 min before MCAO (induced by electrocoagulation) and daily during 3 days. The parameters studied were sensorimotor function, working, object recognition, spatial and aversive memory, cerebral infarct area, myeloperoxidase (MPO) and reduced glutathione (GSH) levels and neurodegeneration through FluoroJade C staining. After MCAO a significant decrease of motor performance and sensory function was found after a neurological evaluation. However, berberine did not improve this neurological deficit. Ischemia caused a 70% increase of infarct area in MCAO group compared with SO, that was decreased by treatment with BE 50 and 100. We observed an increase of vertical exploratory activity (rearings) in the BE 100 group compared to the MCAO. BE 100 treatment also improved MCAO-induced late memory deficits in passive avoidance test (latency - SO: 235.0 ± 33.3s; MCAO: 84.7 ± 23.3s; MCAO + BE100: 300.0 ± 0.0s, p<0.05) and MCAO-induced spatial memory deficits evaluated by water maze test (latency - SO: 10.8 ± 2.4%; MCAO: 23.4 ± 3.9%; MCAO + BE100: 12.8 ± 2.0; p<0.05). BE 50 and 100 treatment significantly prevented the MCAO-induced working memory deficits in y-maze test (spontaneous alternations - SO: 73.8 ± 1.9%; MCAO: 57.2 ± 2.7%; MCAO + BE50: 69.3 ± 3.5; MCAO + BE100: 71.9 ± 3.97%; p<0.05) and object recognition memory deficits (recognition index - SO: 0.51 ± 0.09%; MCAO: 0.068 ± 0.12%; MCAO + BE50: 0.42 ± 0.09%; MCAO + BE100: 0.58 ± 0.16%; p<0.05, Kruskall-Wallis, Mann-Whitney). Neuronal degeneration on berberine-treated groups was significantly less than those submitted to MCAO. Mice submitted to MCAO showed an increase in GSH and MPO levels. BE 100 treatment prevented the increase in MPO activity on striatum (SO: 1.53 ± 0.48; MCAO: 4.89 ± 0.89; MCAO + BE100: 2.52 ± 0.47; p<0.05, ANOVA, Newman-Keuls). Berberine showed a significant protective effect against cerebral ischemia, at least by an anti-inflammatory effect.O acidente vascular cerebral é a segunda principal causa de morte nos países industrializados, sendo comumente dividido em duas categorias: isquêmico e hemorrágico. O mecanismo da lesão isquêmica envolve estresse oxidativo, excitotoxicidade, disfunção mitocondrial, inflamação e apoptose. A Berberina (BE) é um alcalóide derivado do Coptidis rhizom que possui um potente efeito anti-inflamatório e anti-apoptótico. No presente estudo, foi investigado o efeito neuroprotetor da berberina sobre a isquemia cerebral focal (ICF) por oclusão permanente da artéria cerebral média (induzida por eletrocoagulação). Foram utilizados camundongos Swiss machos divididos em cinco grupos (n = 8), dentre eles: Falso operado (FO), ICF e ICF tratados com BE 50 ou 100 mg/kg/dia. BE ou veículo (água destilada) foram administrados por via intragástrica 30 min antes da ICF e diariamente durante 3 dias. Os parâmetros estudados foram função sensório-motora, área de infarto isquêmico, memória de trabalho, reconhecimento de objetos, memória espacial e aversiva, mieloperoxidase (MPO) e glutationa reduzida (GSH), assim como neurodegeneração, através da coloração com FluoroJade C. Os animais submetidos à ICF apresentaram uma diminuição significativa do desempenho motor e função sensorial, no entanto, o tratamento com berberina não diminuiu o déficit neurológico induzido pela isquemia. Verificou-se um aumento significativo da área de infarto nos animais isquemiados, com um aumento de cerca de 70% em relação aos animais falso-operados, sendo esse aumento reduzido pelo tratamento com BE (50 e 100 mg/kg/dia). Observou-se uma diminuição da atividade exploratória vertical (rearings) no grupo submetido à ICF em relação ao grupo FO e uma prevenção desta diminuição pelo tratamento com BE100. O tratamento com BE100 melhorou também os déficits na memória tardia causados pela isquemia, avaliados pelo teste da esquiva passiva (latência - FO: 235,0 ± 33.3s; ICF: 84,7 ± 23.3s; ICF + BE100: 300,0 ± 0.0s, p <0,05) e os déficits de memória espacial, avaliados pelo teste labirinto aquático (latência - FO: 10,8 ± 2,4%; ICF: 23,4 ± 3,9%; ICF + BE100: 12,8 ± 2,0, p <0,05). O tratamento com BE 50 e 100 reduziu de forma significativa os déficits na memória de trabalho, avaliados pelo Y-maze (alternações espontâneas - FO: 73,8 ± 1,9%; ICF: 57,2 ± 2,7%; ICF + BE50: 69,3 ± 3,5; ICF + BE100: 71,9 ± 3,97%, p <0,05), assim como os déficits na memória de reconhecimento de objetos (índice de reconhecimento - FO: 0,51 ± 0,09%; ICF: 0,068 ± 0,12%; ICF + BE50: 0,42 ± 0,09%; ICF+ BE100: 0,58 ± 0,16%, p <0,05, Kruskall-Wallis, Mann-Whitney). A degeneração neuronal nos grupos tratados com berberina foi significativamente menor que nos animais submetidos à ICF. Os animais submetidos à ICF mostraram um aumento nos níveis de GSH e MPO, sendo o tratamento com BE100 capaz de impedir o aumento da atividade da MPO no estriado (FO: 1,53 ± 0,48; ICF: 4,89 ± 0,89; ICF + BE100: 2,52 ± 0,47; p <0,05, ANOVA, Newman-Keuls). A Berberina mostrou um significante efeito neuroprotetor, estando esse efeito relacionado, pelo menos em parte, à atividade anti-inflamatória desse composto.BerberinaIsquemia EncefálicaEstresse OxidativoEfeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanenteinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisporreponame:Repositório Institucional da Universidade Federal do Ceará (UFC)instname:Universidade Federal do Ceará (UFC)instacron:UFCinfo:eu-repo/semantics/openAccessORIGINAL2012_dis_jcsneves.pdf2012_dis_jcsneves.pdfapplication/pdf1548781http://repositorio.ufc.br/bitstream/riufc/4709/1/2012_dis_jcsneves.pdf96ea309aca3044d83f6e31dc7fcd8736MD51LICENSElicense.txtlicense.txttext/plain; charset=utf-81786http://repositorio.ufc.br/bitstream/riufc/4709/2/license.txt8c4401d3d14722a7ca2d07c782a1aab3MD52riufc/47092021-12-20 10:09:43.785oai:repositorio.ufc.br:riufc/4709w4kgbmVjZXNzw6FyaW8gY29uY29yZGFyIGNvbSBhIGxpY2Vuw6dhIGRlIGRpc3RyaWJ1acOnw6NvIG7Do28tZXhjbHVzaXZhLAphbnRlcyBxdWUgbyBkb2N1bWVudG8gcG9zc2EgYXBhcmVjZXIgbm8gUmVwb3NpdMOzcmlvLiBQb3IgZmF2b3IsIGxlaWEgYQpsaWNlbsOnYSBhdGVudGFtZW50ZS4gQ2FzbyBuZWNlc3NpdGUgZGUgYWxndW0gZXNjbGFyZWNpbWVudG8gZW50cmUgZW0KY29udGF0byBhdHJhdsOpcyBkZTogcmVwb3NpdG9yaW9AdWZjLmJyIG91ICg4NSkzMzY2LTk1MDguCgpMSUNFTsOHQSBERSBESVNUUklCVUnDh8ODTyBOw4NPLUVYQ0xVU0lWQQoKQW8gYXNzaW5hciBlIGVudHJlZ2FyIGVzdGEgbGljZW7Dp2EsIG8vYSBTci4vU3JhLiAoYXV0b3Igb3UgZGV0ZW50b3IgZG9zIGRpcmVpdG9zIGRlIGF1dG9yKToKCmEpIENvbmNlZGUgw6AgVW5pdmVyc2lkYWRlIEZlZGVyYWwgZG8gQ2VhcsOhIG8gZGlyZWl0byBuw6NvLWV4Y2x1c2l2byBkZQpyZXByb2R1emlyLCBjb252ZXJ0ZXIgKGNvbW8gZGVmaW5pZG8gYWJhaXhvKSwgY29tdW5pY2FyIGUvb3UKZGlzdHJpYnVpciBvIGRvY3VtZW50byBlbnRyZWd1ZSAoaW5jbHVpbmRvIG8gcmVzdW1vL2Fic3RyYWN0KSBlbQpmb3JtYXRvIGRpZ2l0YWwgb3UgaW1wcmVzc28gZSBlbSBxdWFscXVlciBtZWlvLgoKYikgRGVjbGFyYSBxdWUgbyBkb2N1bWVudG8gZW50cmVndWUgw6kgc2V1IHRyYWJhbGhvIG9yaWdpbmFsLCBlIHF1ZQpkZXTDqW0gbyBkaXJlaXRvIGRlIGNvbmNlZGVyIG9zIGRpcmVpdG9zIGNvbnRpZG9zIG5lc3RhIGxpY2Vuw6dhLiBEZWNsYXJhIHRhbWLDqW0gcXVlIGEgZW50cmVnYSBkbyBkb2N1bWVudG8gbsOjbyBpbmZyaW5nZSwgdGFudG8gcXVhbnRvIGxoZSDDqSBwb3Nzw612ZWwgc2FiZXIsIG9zIGRpcmVpdG9zIGRlIHF1YWxxdWVyIG91dHJhIHBlc3NvYSBvdSBlbnRpZGFkZS4KCmMpIFNlIG8gZG9jdW1lbnRvIGVudHJlZ3VlIGNvbnTDqW0gbWF0ZXJpYWwgZG8gcXVhbCBuw6NvIGRldMOpbSBvcwpkaXJlaXRvcyBkZSBhdXRvciwgZGVjbGFyYSBxdWUgb2J0ZXZlIGF1dG9yaXphw6fDo28gZG8gZGV0ZW50b3IgZG9zCmRpcmVpdG9zIGRlIGF1dG9yIHBhcmEgY29uY2VkZXIgw6AgVW5pdmVyc2lkYWRlIEZlZGVyYWwgZG8gQ2VhcsOhIG9zIGRpcmVpdG9zIHJlcXVlcmlkb3MgcG9yIGVzdGEgbGljZW7Dp2EsIGUgcXVlIGVzc2UgbWF0ZXJpYWwgY3Vqb3MgZGlyZWl0b3Mgc8OjbyBkZSB0ZXJjZWlyb3MgZXN0w6EgY2xhcmFtZW50ZSBpZGVudGlmaWNhZG8gZSByZWNvbmhlY2lkbyBubyB0ZXh0byBvdSBjb250ZcO6ZG8gZG8gZG9jdW1lbnRvIGVudHJlZ3VlLgoKU2UgbyBkb2N1bWVudG8gZW50cmVndWUgw6kgYmFzZWFkbyBlbSB0cmFiYWxobyBmaW5hbmNpYWRvIG91IGFwb2lhZG8KcG9yIG91dHJhIGluc3RpdHVpw6fDo28gcXVlIG7Do28gYSBVbml2ZXJzaWRhZGUgRmVkZXJhbCBkbyBDZWFyw6EsIGRlY2xhcmEgcXVlIGN1bXByaXUgcXVhaXNxdWVyIG9icmlnYcOnw7VlcyBleGlnaWRhcyBwZWxvIHJlc3BlY3Rpdm8gY29udHJhdG8gb3UKYWNvcmRvLgoKQSBVbml2ZXJzaWRhZGUgRmVkZXJhbCBkbyBDZWFyw6EgaWRlbnRpZmljYXLDoSBjbGFyYW1lbnRlIG8ocykgc2V1IChzKSBub21lIChzKSBjb21vIG8gKHMpIGF1dG9yIChlcykgb3UgZGV0ZW50b3IgKGVzKSBkb3MgZGlyZWl0b3MgZG8gZG9jdW1lbnRvIGVudHJlZ3VlLCBlIG7Do28gZmFyw6EgcXVhbHF1ZXIgYWx0ZXJhw6fDo28sIHBhcmEgYWzDqW0gZGFzIHBlcm1pdGlkYXMgcG9yIGVzdGEgbGljZW7Dp2EuCg==Repositório InstitucionalPUBhttp://www.repositorio.ufc.br/ri-oai/requestbu@ufc.br || repositorio@ufc.bropendoar:2021-12-20T13:09:43Repositório Institucional da Universidade Federal do Ceará (UFC) - Universidade Federal do Ceará (UFC)false
dc.title.pt_BR.fl_str_mv Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
title Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
spellingShingle Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
Neves, Julliana Catharina de Sousa
Berberina
Isquemia Encefálica
Estresse Oxidativo
title_short Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
title_full Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
title_fullStr Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
title_full_unstemmed Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
title_sort Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente
author Neves, Julliana Catharina de Sousa
author_facet Neves, Julliana Catharina de Sousa
author_role author
dc.contributor.author.fl_str_mv Neves, Julliana Catharina de Sousa
dc.contributor.advisor1.fl_str_mv Andrade, Geanne Matos de
contributor_str_mv Andrade, Geanne Matos de
dc.subject.por.fl_str_mv Berberina
Isquemia Encefálica
Estresse Oxidativo
topic Berberina
Isquemia Encefálica
Estresse Oxidativo
description Stroke is the second leading cause death in industrialized countries and can be subdivided into 2 categories, ischemic and hemorrhagic. The mechanisms of ischemic brain damage involve oxidative stress, excitotoxicity, mitochondrial dysfunction, inflammation and apoptosis. Berberine (BE) is an alkaloid derived from Coptidis rhizom which has potent anti-inflammatory and anti-apoptotic effects. In present study, the neuroprotector effect of berberine after permanent middle cerebral artery occlusion (MCAO) was investigated. Male Swiss mice were divided into five groups (n=8): Sham operated (SO), MCAO, BE 50 and 100mg/kg/day plus MCAO. BE or vehicle (distilled water) were administrated intragastrically 30 min before MCAO (induced by electrocoagulation) and daily during 3 days. The parameters studied were sensorimotor function, working, object recognition, spatial and aversive memory, cerebral infarct area, myeloperoxidase (MPO) and reduced glutathione (GSH) levels and neurodegeneration through FluoroJade C staining. After MCAO a significant decrease of motor performance and sensory function was found after a neurological evaluation. However, berberine did not improve this neurological deficit. Ischemia caused a 70% increase of infarct area in MCAO group compared with SO, that was decreased by treatment with BE 50 and 100. We observed an increase of vertical exploratory activity (rearings) in the BE 100 group compared to the MCAO. BE 100 treatment also improved MCAO-induced late memory deficits in passive avoidance test (latency - SO: 235.0 ± 33.3s; MCAO: 84.7 ± 23.3s; MCAO + BE100: 300.0 ± 0.0s, p<0.05) and MCAO-induced spatial memory deficits evaluated by water maze test (latency - SO: 10.8 ± 2.4%; MCAO: 23.4 ± 3.9%; MCAO + BE100: 12.8 ± 2.0; p<0.05). BE 50 and 100 treatment significantly prevented the MCAO-induced working memory deficits in y-maze test (spontaneous alternations - SO: 73.8 ± 1.9%; MCAO: 57.2 ± 2.7%; MCAO + BE50: 69.3 ± 3.5; MCAO + BE100: 71.9 ± 3.97%; p<0.05) and object recognition memory deficits (recognition index - SO: 0.51 ± 0.09%; MCAO: 0.068 ± 0.12%; MCAO + BE50: 0.42 ± 0.09%; MCAO + BE100: 0.58 ± 0.16%; p<0.05, Kruskall-Wallis, Mann-Whitney). Neuronal degeneration on berberine-treated groups was significantly less than those submitted to MCAO. Mice submitted to MCAO showed an increase in GSH and MPO levels. BE 100 treatment prevented the increase in MPO activity on striatum (SO: 1.53 ± 0.48; MCAO: 4.89 ± 0.89; MCAO + BE100: 2.52 ± 0.47; p<0.05, ANOVA, Newman-Keuls). Berberine showed a significant protective effect against cerebral ischemia, at least by an anti-inflammatory effect.
publishDate 2012
dc.date.issued.fl_str_mv 2012
dc.date.accessioned.fl_str_mv 2013-03-15T12:32:48Z
dc.date.available.fl_str_mv 2013-03-15T12:32:48Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/masterThesis
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status_str publishedVersion
dc.identifier.citation.fl_str_mv NEVES, J. C. S. Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente. 2012. 98 f. Dissertação (Mestrado em Farmacologia) - Faculdade de Farmácia, Odontologia e Enfermagem, Universidade Federal do Ceará, Fortaleza, 2012.
dc.identifier.uri.fl_str_mv http://www.repositorio.ufc.br/handle/riufc/4709
identifier_str_mv NEVES, J. C. S. Efeito protetor da berberina no dano cerebral, deficit de memória, estresse oxidativo e inflamação de camundongos submetidos à isquemia cerebral focal permanente. 2012. 98 f. Dissertação (Mestrado em Farmacologia) - Faculdade de Farmácia, Odontologia e Enfermagem, Universidade Federal do Ceará, Fortaleza, 2012.
url http://www.repositorio.ufc.br/handle/riufc/4709
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