Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas

Abrantes, Antonia Fernandes Furtado de

Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas

Detalhes bibliográficos
Ano de defesa:	2024
Autor(a) principal:	Abrantes, Antonia Fernandes Furtado de
Orientador(a):	Não Informado pela instituição
Banca de defesa:	Não Informado pela instituição
Tipo de documento:	Tese
Tipo de acesso:	Acesso aberto
Idioma:	por
Instituição de defesa:	Universidade Federal da Paraíba Brasil Psicologia Programa de Pós-Graduação em Neurociência Cognitiva e Comportamento UFPB
Programa de Pós-Graduação:	Não Informado pela instituição
Departamento:	Não Informado pela instituição
País:	Não Informado pela instituição
Palavras-chave em Português:	Depressão o-Eugenol - Atividade antidepressiva Dexametasona Antidepressivos - mecanismos de ação Avaliação toxicológica Depression Dexamethasone Mechanisms of action Toxicological assessment CNPQ::CIENCIAS HUMANAS::PSICOLOGIA
Link de acesso:	https://repositorio.ufpb.br/jspui/handle/123456789/34310
Resumo:	Major depressive disorder (MDD) is a common and debilitating mental disorder, with women almost twice as likely to develop the disease as men. Conventional treatment options have side effects and questionable efficacy, requiring the search for new, more effective and safer drugs. The present study investigated pharmacokinetic parameters and in silico toxicity, acute and subacute toxicity in vivo, and the antidepressant-like activity of o-eugenol administered in repeated doses, in a behavioral animal model of depression induced by repeated administra-tion of dexamethasone in female mice. In the in silico study, pkCSM and SwissADME virtual platforms were used. In the in vivo studies, acute and repeated-dose oral toxicity were per-formed following the protocols of the Organization of Economic Cooperation and Develop-ment (OECD), through the observation of behavioral, weight, feeding, anatomopathological, and hematological and biochemical parameters in the subacute part. In the investigation of the antidepressant-like activity of o-eugenol, orally, behavioral tests of forced swimming (FST), tail suspension (TST) and sucrose preference (SPT) were performed, in addition to the rota-rod to evaluate motor coordination. The effect of o-eugenol on the seizure threshold and its synergism with imipramine were studied, oxidative stress parameters, IL-1β levels and metabolomic study by nuclear magnetic resonance technique were evaluated. As in silico re-sults, o-eugenol showed good oral absorption, permeability to the blood-brain barrier and the central nervous system, was not a substrate for other products and did not show toxic respons-es in predictive models. In vivo studies, in acute and repeated dose toxicity, o-eugenol did not promote significant changes in most of the parameters investigated. The estimated acute lethal dose (LD50) was 1000 mg/kg. From the pharmacological screening, the three doses of o-eugenol (25, 50 and 100 mg/kg) used in the study were determined. The o-eugenol did not alter the motor coordination of the animals in the rota-rod test (p>0,05). In the FST and TST tests, dexamethasone increased the immobility time and decreased the latency to immobility of the mice in relation to the control, while o-eugenol and imipramine decreased the immo-bility time and increased the latency to immobility in relation to dexamethasone (p<0,05). In the SPT, dexamethasone decreased sucrose preference of the animals, while o-eugenol and imipramine reversed the behavior (p<0,05). The o-eugenol reduced lipid peroxidation and increased the levels of the antioxidant glutathione in brain structures, and decreased serum levels of IL-1β (p<0.05). In the metabolomic study performed in the hippocampus, there were no significant differences between the groups according to PCA analysis. Pretreatment with o-eugenol did not decrease the latency to the first seizure in animals that received a subconvul-sive dose of 35 mg/kg of pentylenetetrazol (p<0.05) and a synergistic interaction between imipramine and o-eugenol was suggested (p<0.05). Thus, the findings demonstrated that o-eugenol presented relatively low toxicity, showed an effect similar to the antidepressant imi-pramine with a decrease in oxidative stress in brain structures, a decrease in serum levels of IL-1β, and also had a synergistic effect with imipramine, but was devoid of proconvulsant adverse effects.

Metadados do item

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spelling	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeasDepressãoo-Eugenol - Atividade antidepressivaDexametasonaAntidepressivos - mecanismos de açãoAvaliação toxicológicaDepressionDexamethasoneMechanisms of actionToxicological assessmentCNPQ::CIENCIAS HUMANAS::PSICOLOGIAMajor depressive disorder (MDD) is a common and debilitating mental disorder, with women almost twice as likely to develop the disease as men. Conventional treatment options have side effects and questionable efficacy, requiring the search for new, more effective and safer drugs. The present study investigated pharmacokinetic parameters and in silico toxicity, acute and subacute toxicity in vivo, and the antidepressant-like activity of o-eugenol administered in repeated doses, in a behavioral animal model of depression induced by repeated administra-tion of dexamethasone in female mice. In the in silico study, pkCSM and SwissADME virtual platforms were used. In the in vivo studies, acute and repeated-dose oral toxicity were per-formed following the protocols of the Organization of Economic Cooperation and Develop-ment (OECD), through the observation of behavioral, weight, feeding, anatomopathological, and hematological and biochemical parameters in the subacute part. In the investigation of the antidepressant-like activity of o-eugenol, orally, behavioral tests of forced swimming (FST), tail suspension (TST) and sucrose preference (SPT) were performed, in addition to the rota-rod to evaluate motor coordination. The effect of o-eugenol on the seizure threshold and its synergism with imipramine were studied, oxidative stress parameters, IL-1β levels and metabolomic study by nuclear magnetic resonance technique were evaluated. As in silico re-sults, o-eugenol showed good oral absorption, permeability to the blood-brain barrier and the central nervous system, was not a substrate for other products and did not show toxic respons-es in predictive models. In vivo studies, in acute and repeated dose toxicity, o-eugenol did not promote significant changes in most of the parameters investigated. The estimated acute lethal dose (LD50) was 1000 mg/kg. From the pharmacological screening, the three doses of o-eugenol (25, 50 and 100 mg/kg) used in the study were determined. The o-eugenol did not alter the motor coordination of the animals in the rota-rod test (p>0,05). In the FST and TST tests, dexamethasone increased the immobility time and decreased the latency to immobility of the mice in relation to the control, while o-eugenol and imipramine decreased the immo-bility time and increased the latency to immobility in relation to dexamethasone (p<0,05). In the SPT, dexamethasone decreased sucrose preference of the animals, while o-eugenol and imipramine reversed the behavior (p<0,05). The o-eugenol reduced lipid peroxidation and increased the levels of the antioxidant glutathione in brain structures, and decreased serum levels of IL-1β (p<0.05). In the metabolomic study performed in the hippocampus, there were no significant differences between the groups according to PCA analysis. Pretreatment with o-eugenol did not decrease the latency to the first seizure in animals that received a subconvul-sive dose of 35 mg/kg of pentylenetetrazol (p<0.05) and a synergistic interaction between imipramine and o-eugenol was suggested (p<0.05). Thus, the findings demonstrated that o-eugenol presented relatively low toxicity, showed an effect similar to the antidepressant imi-pramine with a decrease in oxidative stress in brain structures, a decrease in serum levels of IL-1β, and also had a synergistic effect with imipramine, but was devoid of proconvulsant adverse effects.NenhumaO transtorno depressivo maior (TDM) é um transtorno mental comun e debilitante, sendo as mulheres quase duas vezes mais propensas a desenvolverem a doença que os homens. As op-ções de tratamento convencionais possuem efeitos colaterais e eficácia questionável, sendo necessária a busca de novos medicamentos mais eficazes e seguros. O presente estudo inves-tigou parâmetros farmacocinéticos e toxicidade in silico, toxicidade aguda e subaguda in vivo, e a atividade antidepressiva-símile do o-eugenol administrado em doses repetidas, em modelo animal comportamental de depressão induzido por administração repetida de dexametasona em camundongos fêmeas. No estudo in silico, foram utilizadas plataformas virtuais pkCSM e SwissADME. Nos estudos in vivo, toxicidade aguda e de doses repetidas por via oral foram realizados seguindo os protocolos da Organisation of Economic Cooperation and Deve-lopment (OECD), através da observação de parâmetros comportamentais, ponderais, alimen-tares, anatomopatológicos, além de hematológicos, bioquímicos na parte subaguda. Na inves-tigação da atividade antidepressiva-símile do o-eugenol, por via oral, foram realizados testes comportamentais do nado forçado (TNF), suspensão da cauda (TSC) e preferência pela saca-rose (TPS), além do rota-rod para avaliar a coordenação motora. Foi estudado o efeito do o-eugenol no limiar de convulsões e seu sinergismo com a imipramina, avaliado parâmetros de estresse oxidativo, níveis de IL-1β e estudo metabolômico pela técnica de ressonância magné-tica nuclear. Como resultados in sílico, o-eugenol apresentou boa absorção via oral, permeabi-lidade a barreira hemato encefálica e ao sistema nervoso central, não foi substrato para outros produtos e não apresentou respostas tóxicas nos modelos preditivos. Nos estudos in vivo, na toxicidade aguda e de doses repetidas, o o-eugenol não promoveu alterações significativas na maioria dos parâmetros investigados. A estimativa da dose aguda letal (DL50) foi de 1000 mg/kg. A partir da triagem farmacológica foi determinado as três doses de o-eugenol (25, 50 e 100 mg/kg) utilizadas no estudo. O o-eugenol não alterou a coordenação motora dos animais no teste do rota-rod (p>0,05). Nos testes TNF e TSC, a dexametasona aumentou o tempo de imobilidade e diminuiu a latência para imobilidade dos camundongos em relação ao controle, enquanto o-eugenol e a imipramina diminuíram o tempo de imobilidade e aumentaram a la-tência para imobilidade em relação a dexametasona (p<0,05). No TPS, a dexametasona dimi-nuiu a preferência à sacarose dos animais, enquanto o-eugenol e a imipramina reverteu o comportamento (p<0,05). O o-eugenol reduziu a peroxidação lipídica e aumentou os níveis do antioxidante glutationa em estruturas cerebrais, e diminuiu os níveis séricos de IL-1β (p<0,05). No estudo metabolômico, feito no hipocampo, não houve diferenças importantes entre os grupos pela análise do PCA. O pré-tratamento com o-eugenol não diminuiu a latência para a primeira convulsão dos animais que receberam dose subconvulsiva 35mg/kg de penti-lenotetrazol (p<0,05) e foi sugestivo uma interação sinérgica entre a imipramina e o-eugenol (p<0,05). Assim, os achados demonstraram que o o-eugenol apresentou toxicidade relativa-mente baixa, mostrou efeito semelhante ao antidepressivo imipramina com diminuição do estresse oxidativo em estruturas cerebrais, diminuição dos níveis séricos de IL-1β, além de também ter efeito sinérgico com a imipramina, mas ser desprovido de efeito adverso pró-convulsivante.Universidade Federal da ParaíbaBrasilPsicologiaPrograma de Pós-Graduação em Neurociência Cognitiva e ComportamentoUFPBSalvadori, Mirian Graciela da Silva Stiebbehttp://lattes.cnpq.br/2669989944106416Abrantes, Antonia Fernandes Furtado de2025-04-23T11:04:43Z2024-12-032025-04-23T11:04:43Z2024-11-08info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesishttps://repositorio.ufpb.br/jspui/handle/123456789/34310porAttribution-NoDerivs 3.0 Brazilhttp://creativecommons.org/licenses/by-nd/3.0/br/info:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFPBinstname:Universidade Federal da Paraíba (UFPB)instacron:UFPB2025-04-24T06:10:46Zoai:repositorio.ufpb.br:123456789/34310Repositório InstitucionalPUBhttps://repositorio.ufpb.br/oai/requestdiretoria@ufpb.br\|\|bdtd@biblioteca.ufpb.bropendoar:25462025-04-24T06:10:46Repositório Institucional da UFPB - Universidade Federal da Paraíba (UFPB)false
dc.title.none.fl_str_mv	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
title	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
spellingShingle	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas Abrantes, Antonia Fernandes Furtado de Depressão o-Eugenol - Atividade antidepressiva Dexametasona Antidepressivos - mecanismos de ação Avaliação toxicológica Depression Dexamethasone Mechanisms of action Toxicological assessment CNPQ::CIENCIAS HUMANAS::PSICOLOGIA
title_short	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
title_full	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
title_fullStr	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
title_full_unstemmed	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
title_sort	Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas
author	Abrantes, Antonia Fernandes Furtado de
author_facet	Abrantes, Antonia Fernandes Furtado de
author_role	author
dc.contributor.none.fl_str_mv	Salvadori, Mirian Graciela da Silva Stiebbe http://lattes.cnpq.br/2669989944106416
dc.contributor.author.fl_str_mv	Abrantes, Antonia Fernandes Furtado de
dc.subject.por.fl_str_mv	Depressão o-Eugenol - Atividade antidepressiva Dexametasona Antidepressivos - mecanismos de ação Avaliação toxicológica Depression Dexamethasone Mechanisms of action Toxicological assessment CNPQ::CIENCIAS HUMANAS::PSICOLOGIA
topic	Depressão o-Eugenol - Atividade antidepressiva Dexametasona Antidepressivos - mecanismos de ação Avaliação toxicológica Depression Dexamethasone Mechanisms of action Toxicological assessment CNPQ::CIENCIAS HUMANAS::PSICOLOGIA
description	Major depressive disorder (MDD) is a common and debilitating mental disorder, with women almost twice as likely to develop the disease as men. Conventional treatment options have side effects and questionable efficacy, requiring the search for new, more effective and safer drugs. The present study investigated pharmacokinetic parameters and in silico toxicity, acute and subacute toxicity in vivo, and the antidepressant-like activity of o-eugenol administered in repeated doses, in a behavioral animal model of depression induced by repeated administra-tion of dexamethasone in female mice. In the in silico study, pkCSM and SwissADME virtual platforms were used. In the in vivo studies, acute and repeated-dose oral toxicity were per-formed following the protocols of the Organization of Economic Cooperation and Develop-ment (OECD), through the observation of behavioral, weight, feeding, anatomopathological, and hematological and biochemical parameters in the subacute part. In the investigation of the antidepressant-like activity of o-eugenol, orally, behavioral tests of forced swimming (FST), tail suspension (TST) and sucrose preference (SPT) were performed, in addition to the rota-rod to evaluate motor coordination. The effect of o-eugenol on the seizure threshold and its synergism with imipramine were studied, oxidative stress parameters, IL-1β levels and metabolomic study by nuclear magnetic resonance technique were evaluated. As in silico re-sults, o-eugenol showed good oral absorption, permeability to the blood-brain barrier and the central nervous system, was not a substrate for other products and did not show toxic respons-es in predictive models. In vivo studies, in acute and repeated dose toxicity, o-eugenol did not promote significant changes in most of the parameters investigated. The estimated acute lethal dose (LD50) was 1000 mg/kg. From the pharmacological screening, the three doses of o-eugenol (25, 50 and 100 mg/kg) used in the study were determined. The o-eugenol did not alter the motor coordination of the animals in the rota-rod test (p>0,05). In the FST and TST tests, dexamethasone increased the immobility time and decreased the latency to immobility of the mice in relation to the control, while o-eugenol and imipramine decreased the immo-bility time and increased the latency to immobility in relation to dexamethasone (p<0,05). In the SPT, dexamethasone decreased sucrose preference of the animals, while o-eugenol and imipramine reversed the behavior (p<0,05). The o-eugenol reduced lipid peroxidation and increased the levels of the antioxidant glutathione in brain structures, and decreased serum levels of IL-1β (p<0.05). In the metabolomic study performed in the hippocampus, there were no significant differences between the groups according to PCA analysis. Pretreatment with o-eugenol did not decrease the latency to the first seizure in animals that received a subconvul-sive dose of 35 mg/kg of pentylenetetrazol (p<0.05) and a synergistic interaction between imipramine and o-eugenol was suggested (p<0.05). Thus, the findings demonstrated that o-eugenol presented relatively low toxicity, showed an effect similar to the antidepressant imi-pramine with a decrease in oxidative stress in brain structures, a decrease in serum levels of IL-1β, and also had a synergistic effect with imipramine, but was devoid of proconvulsant adverse effects.
publishDate	2024
dc.date.none.fl_str_mv	2024-12-03 2024-11-08 2025-04-23T11:04:43Z 2025-04-23T11:04:43Z
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	https://repositorio.ufpb.br/jspui/handle/123456789/34310
url	https://repositorio.ufpb.br/jspui/handle/123456789/34310
dc.language.iso.fl_str_mv	por
language	por
dc.rights.driver.fl_str_mv	Attribution-NoDerivs 3.0 Brazil http://creativecommons.org/licenses/by-nd/3.0/br/ info:eu-repo/semantics/openAccess
rights_invalid_str_mv	Attribution-NoDerivs 3.0 Brazil http://creativecommons.org/licenses/by-nd/3.0/br/
eu_rights_str_mv	openAccess
dc.publisher.none.fl_str_mv	Universidade Federal da Paraíba Brasil Psicologia Programa de Pós-Graduação em Neurociência Cognitiva e Comportamento UFPB
publisher.none.fl_str_mv	Universidade Federal da Paraíba Brasil Psicologia Programa de Pós-Graduação em Neurociência Cognitiva e Comportamento UFPB
dc.source.none.fl_str_mv	reponame:Repositório Institucional da UFPB instname:Universidade Federal da Paraíba (UFPB) instacron:UFPB
instname_str	Universidade Federal da Paraíba (UFPB)
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reponame_str	Repositório Institucional da UFPB
collection	Repositório Institucional da UFPB
repository.name.fl_str_mv	Repositório Institucional da UFPB - Universidade Federal da Paraíba (UFPB)
repository.mail.fl_str_mv	diretoria@ufpb.br\|\|bdtd@biblioteca.ufpb.br
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Investigação da toxicidade e atividade antidepressiva-símile do o-Eugenol em camundongos fêmeas

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