Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve

Detalhes bibliográficos
Ano de defesa: 2021
Autor(a) principal: Furtado, Andrezza Bond Vieira
Orientador(a): Não Informado pela instituição
Banca de defesa: Não Informado pela instituição
Tipo de documento: Tese
Tipo de acesso: Acesso aberto
dARK ID: ark:/26339/0013000014ftb
Idioma: por
Instituição de defesa: Universidade Federal de Santa Maria
Brasil
Bioquímica
UFSM
Programa de Pós-Graduação em Ciências Biológicas: Bioquímica Toxicológica
Centro de Ciências Naturais e Exatas
Programa de Pós-Graduação: Não Informado pela instituição
Departamento: Não Informado pela instituição
País: Não Informado pela instituição
Palavras-chave em Português:
Neuroproteção
Neurodegeneração
Droga multi-alvo
Neuroinflamação
Disfunção mitocondrial
Sobrevivência neuronal
Neuroprotection
Neurodegeneration
Multi-target drug
Neuroinflammation
Mitochondrial dysfunction
Neuronal survival
CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA
Link de acesso: http://repositorio.ufsm.br/handle/1/24412
Resumo: Traumatic brain injury (TBI) is a multisystemic pathology with interactions between central nervous system, peripheral nervous system and immune system. It is one of the main causes of death and desability worldwide. The pathophysiology of TBI involves cell death pathways and tissue loss that lead to neurodegeneration and deficits in neurological function. It is estimated that 75 to 90% of TBI cases are classified as mild, and the damage following TBI may be underestimated. Despite the large numbers of TBI cases, there is no effective pharmacological treatment available. This study aimed to investigate the effects on TBI outcomes of the new hybrid molecule 3-ethoxycarbonyl-2-methyl-4-(2-nitrophenyl)-4,11-dihydro1H-pyrido[2,3-b][1,5]benzodiazepine (JM-20). JM-20 emerge as a neuroprotective drug because it targets mediators involved in cell death events: calcium channels, due to the dihydropyridine portion; and GABAa receptors, due to benzodiazepine action. Male Wistar rats were submitted to a weight drop model of mild TBI and treated with a single dose of JM-20 (8 mg/kg). 24 h following TBI, JM-20 treatment was able to attenuate locomotor and short-term memory deficits; decrease brain edema; avoid the exacerbated activation of glial cells and consequently the pro-inflammatory signaling by decreasing release of pro-inflammatory cytokines and higher release of neurotrophins; avoid mitochondrial dysfunction through increased oxygen flux consumption in oxidative phosphorylation, and then, improve mitochondrial functionality; JM-20 treatment was also able to mantain the activation of an important pathway related to cellular cascades. Based on these, is possible to confirm that JM-20 has neuroprotective effects by modulating important secondary injury targets and corroborate our hypothesis that JM-20 may become a promising treatment strategy to TBI.
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repository_id_str
spelling Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leveNeuroprotective effect of JM-20 in rats submitted to mild traumatic brain injuryNeuroproteçãoNeurodegeneraçãoDroga multi-alvoNeuroinflamaçãoDisfunção mitocondrialSobrevivência neuronalNeuroprotectionNeurodegenerationMulti-target drugNeuroinflammationMitochondrial dysfunctionNeuronal survivalCNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICATraumatic brain injury (TBI) is a multisystemic pathology with interactions between central nervous system, peripheral nervous system and immune system. It is one of the main causes of death and desability worldwide. The pathophysiology of TBI involves cell death pathways and tissue loss that lead to neurodegeneration and deficits in neurological function. It is estimated that 75 to 90% of TBI cases are classified as mild, and the damage following TBI may be underestimated. Despite the large numbers of TBI cases, there is no effective pharmacological treatment available. This study aimed to investigate the effects on TBI outcomes of the new hybrid molecule 3-ethoxycarbonyl-2-methyl-4-(2-nitrophenyl)-4,11-dihydro1H-pyrido[2,3-b][1,5]benzodiazepine (JM-20). JM-20 emerge as a neuroprotective drug because it targets mediators involved in cell death events: calcium channels, due to the dihydropyridine portion; and GABAa receptors, due to benzodiazepine action. Male Wistar rats were submitted to a weight drop model of mild TBI and treated with a single dose of JM-20 (8 mg/kg). 24 h following TBI, JM-20 treatment was able to attenuate locomotor and short-term memory deficits; decrease brain edema; avoid the exacerbated activation of glial cells and consequently the pro-inflammatory signaling by decreasing release of pro-inflammatory cytokines and higher release of neurotrophins; avoid mitochondrial dysfunction through increased oxygen flux consumption in oxidative phosphorylation, and then, improve mitochondrial functionality; JM-20 treatment was also able to mantain the activation of an important pathway related to cellular cascades. Based on these, is possible to confirm that JM-20 has neuroprotective effects by modulating important secondary injury targets and corroborate our hypothesis that JM-20 may become a promising treatment strategy to TBI.Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPESO traumatismo cranioencefálico (TCE) é uma patologia multissistêmica que envolve interações entre o sistema nervoso central, o sistema nervoso periférico e o sistema imune, sendo uma das principais causas de morte e de condições incapacitantes no mundo. A fisiopatologia do TCE envolve mecanismos complexos relacionados à morte celular e à perda tecidual, que levam à neurodegeneração e a déficits na função neurológica. Estima-se que 75 a 90% dos casos de TCE sejam classificados como leves e gerem danos que podem ser subestimados. Apesar da sua alta incidência, ainda não há tratamento farmacológico padrão para essa patologia. Nesse contexto, a molécula 3- etoxicarbonil-2-metil-4-(2-nitrofenil)-4,11-di-hidro-1H-pirido[2,3-b][1,5] benzodiazepina (JM-20) surge como uma droga neuroprotetora por possuir, como alvo, mediadores envolvidos em eventos de morte celular: os canais de cálcio, devido à porção di-hidropirídinica; e os receptores GABAa, devido à ação benzodiazepínica. Neste estudo, investigamos os efeitos neuroprotetores do tratamento com JM-20 (8 mg/kg) administrado 1h após o modelo de queda de peso em ratos Wistar. O tratamento com JM-20 24h após TCE leve foi capaz de atenuar déficits na locomoção e na memória de curto prazo; diminuir o edema cerebral; controlar a ativação exacerbada das células gliais e, consequentemente, a sinalização pró-inflamatória, comprovada pela menor liberação de citocinas pró-inflamatórias e pela maior liberação de neurotrofinas; evitar a disfunção mitocondrial, através de maior consumo do fluxo de oxigênio durante a fosforilação oxidativa e, com base nisso, melhorar um parâmetro relacionado à funcionalidade mitocondrial; e, ainda, preservar a ativação de uma importante via relacionada a cascatas de sobrevivência celular. Com base nos resultados aqui obtidos, pode-se dizer que o JM-20 apresentou efeitos neuroprotetores ao atuar em importantes pontos da lesão secundária induzida por TCE, tornando-se, dessa maneira, um composto com potencial para uso no tratamento do TCE.Universidade Federal de Santa MariaBrasilBioquímicaUFSMPrograma de Pós-Graduação em Ciências Biológicas: Bioquímica ToxicológicaCentro de Ciências Naturais e ExatasSoares, Félix Alexandre Antuneshttp://lattes.cnpq.br/8752453650114092Royes, Luiz Fernando FreireRubin, Maribel AntonelloOliveira, Mauro SchneiderKlamt, FábioFranco, Jeferson LuisFurtado, Andrezza Bond Vieira2022-05-23T14:42:13Z2022-05-23T14:42:13Z2021-09-10info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesisapplication/pdfhttp://repositorio.ufsm.br/handle/1/24412ark:/26339/0013000014ftbporAttribution-NonCommercial-NoDerivatives 4.0 Internationalinfo:eu-repo/semantics/openAccessreponame:Manancial - Repositório Digital da UFSMinstname:Universidade Federal de Santa Maria (UFSM)instacron:UFSM2022-05-23T14:43:00Zoai:repositorio.ufsm.br:1/24412Biblioteca Digital de Teses e Dissertaçõeshttps://repositorio.ufsm.br/PUBhttps://repositorio.ufsm.br/oai/requestatendimento.sib@ufsm.br||tedebc@gmail.com||manancial@ufsm.bropendoar:2022-05-23T14:43Manancial - Repositório Digital da UFSM - Universidade Federal de Santa Maria (UFSM)false
dc.title.none.fl_str_mv Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
Neuroprotective effect of JM-20 in rats submitted to mild traumatic brain injury
title Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
spellingShingle Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
Furtado, Andrezza Bond Vieira
Neuroproteção
Neurodegeneração
Droga multi-alvo
Neuroinflamação
Disfunção mitocondrial
Sobrevivência neuronal
Neuroprotection
Neurodegeneration
Multi-target drug
Neuroinflammation
Mitochondrial dysfunction
Neuronal survival
CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA
title_short Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
title_full Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
title_fullStr Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
title_full_unstemmed Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
title_sort Efeito neuroprotetor do JM-20 em ratos submetidos a traumatismo cranioencefálico leve
author Furtado, Andrezza Bond Vieira
author_facet Furtado, Andrezza Bond Vieira
author_role author
dc.contributor.none.fl_str_mv Soares, Félix Alexandre Antunes
http://lattes.cnpq.br/8752453650114092
Royes, Luiz Fernando Freire
Rubin, Maribel Antonello
Oliveira, Mauro Schneider
Klamt, Fábio
Franco, Jeferson Luis
dc.contributor.author.fl_str_mv Furtado, Andrezza Bond Vieira
dc.subject.por.fl_str_mv Neuroproteção
Neurodegeneração
Droga multi-alvo
Neuroinflamação
Disfunção mitocondrial
Sobrevivência neuronal
Neuroprotection
Neurodegeneration
Multi-target drug
Neuroinflammation
Mitochondrial dysfunction
Neuronal survival
CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA
topic Neuroproteção
Neurodegeneração
Droga multi-alvo
Neuroinflamação
Disfunção mitocondrial
Sobrevivência neuronal
Neuroprotection
Neurodegeneration
Multi-target drug
Neuroinflammation
Mitochondrial dysfunction
Neuronal survival
CNPQ::CIENCIAS BIOLOGICAS::BIOQUIMICA
description Traumatic brain injury (TBI) is a multisystemic pathology with interactions between central nervous system, peripheral nervous system and immune system. It is one of the main causes of death and desability worldwide. The pathophysiology of TBI involves cell death pathways and tissue loss that lead to neurodegeneration and deficits in neurological function. It is estimated that 75 to 90% of TBI cases are classified as mild, and the damage following TBI may be underestimated. Despite the large numbers of TBI cases, there is no effective pharmacological treatment available. This study aimed to investigate the effects on TBI outcomes of the new hybrid molecule 3-ethoxycarbonyl-2-methyl-4-(2-nitrophenyl)-4,11-dihydro1H-pyrido[2,3-b][1,5]benzodiazepine (JM-20). JM-20 emerge as a neuroprotective drug because it targets mediators involved in cell death events: calcium channels, due to the dihydropyridine portion; and GABAa receptors, due to benzodiazepine action. Male Wistar rats were submitted to a weight drop model of mild TBI and treated with a single dose of JM-20 (8 mg/kg). 24 h following TBI, JM-20 treatment was able to attenuate locomotor and short-term memory deficits; decrease brain edema; avoid the exacerbated activation of glial cells and consequently the pro-inflammatory signaling by decreasing release of pro-inflammatory cytokines and higher release of neurotrophins; avoid mitochondrial dysfunction through increased oxygen flux consumption in oxidative phosphorylation, and then, improve mitochondrial functionality; JM-20 treatment was also able to mantain the activation of an important pathway related to cellular cascades. Based on these, is possible to confirm that JM-20 has neuroprotective effects by modulating important secondary injury targets and corroborate our hypothesis that JM-20 may become a promising treatment strategy to TBI.
publishDate 2021
dc.date.none.fl_str_mv 2021-09-10
2022-05-23T14:42:13Z
2022-05-23T14:42:13Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/doctoralThesis
format doctoralThesis
status_str publishedVersion
dc.identifier.uri.fl_str_mv http://repositorio.ufsm.br/handle/1/24412
dc.identifier.dark.fl_str_mv ark:/26339/0013000014ftb
url http://repositorio.ufsm.br/handle/1/24412
identifier_str_mv ark:/26339/0013000014ftb
dc.language.iso.fl_str_mv por
language por
dc.rights.driver.fl_str_mv Attribution-NonCommercial-NoDerivatives 4.0 International
info:eu-repo/semantics/openAccess
rights_invalid_str_mv Attribution-NonCommercial-NoDerivatives 4.0 International
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.publisher.none.fl_str_mv Universidade Federal de Santa Maria
Brasil
Bioquímica
UFSM
Programa de Pós-Graduação em Ciências Biológicas: Bioquímica Toxicológica
Centro de Ciências Naturais e Exatas
publisher.none.fl_str_mv Universidade Federal de Santa Maria
Brasil
Bioquímica
UFSM
Programa de Pós-Graduação em Ciências Biológicas: Bioquímica Toxicológica
Centro de Ciências Naturais e Exatas
dc.source.none.fl_str_mv reponame:Manancial - Repositório Digital da UFSM
instname:Universidade Federal de Santa Maria (UFSM)
instacron:UFSM
instname_str Universidade Federal de Santa Maria (UFSM)
instacron_str UFSM
institution UFSM
reponame_str Manancial - Repositório Digital da UFSM
collection Manancial - Repositório Digital da UFSM
repository.name.fl_str_mv Manancial - Repositório Digital da UFSM - Universidade Federal de Santa Maria (UFSM)
repository.mail.fl_str_mv atendimento.sib@ufsm.br||tedebc@gmail.com||manancial@ufsm.br
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