Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado

Detalhes bibliográficos
Ano de defesa: 2010
Autor(a) principal: Gianlorenço, Anna Carolyna Lepesteur
Orientador(a): Mattioli, Rosana lattes
Banca de defesa: Não Informado pela instituição
Tipo de documento: Dissertação
Tipo de acesso: Acesso aberto
Idioma: por
Instituição de defesa: Universidade Federal de São Carlos
Programa de Pós-Graduação: Programa de Pós-Graduação em Fisioterapia - PPGFt
Departamento: Não Informado pela instituição
País: BR
Palavras-chave em Português:
Ansiedade
Aprendizagem e memória
L-Histidina
Clorfeniramina
Labirinto em cruz elevado
Área do conhecimento CNPq:
CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL
Link de acesso: https://repositorio.ufscar.br/handle/20.500.14289/5259
Resumo: The aim of this study was to assess the influence of histaminergic substances on anxiety and emotional memory in mice exposed and re-exposed to the Elevated Plus-Maze (EPM). For this, two experiments were conducted. Experiment 1 evaluated the effects of L-histidine on anxiety and emotional memory and contribution of the H 1 antagonist (chlorpheniramine) for these effects. Experiment 2 evaluated the effect of chronic treatment with chlorpheniramine (CPA) on anxiety and emotional memory. The experiments were performed with Swiss-albino mice (25-35g), using the model of the EPM in two consecutive days, exposure (T1) and reexposure (T2). In experiment 1, animals received combined intraperitoneal injection pretrial in T1: SAL/SAL (saline + saline), LH/SAL (L-histidine 500mg/kg + saline) and LH/CPA (Lhistidine + Chlorpheniramine 16mg/kg). The combined injection was executed by one first injection, followed by a second injection 30 minutes later. The test was performed in the EPM 10 minutes after the last injection. Each animal was positioned on the center platform of the maze facing the open arm and had five minutes to explore. After 24 hours (T2), the animals received the same pharmacological treatment of the previous day and were re-exposed to the EPM, following the procedures described. In experiment 2, the procedure was the application of chronic injections of SAL or CPA, intraperitoneally (i.p.) for 15 days. After this period, on the first day of test (T1), the animals were injected i.p. with SAL or CPA and 40 minutes later were exposed to EPM for 5 minutes. In T2, the animals received the same pharmacological treatment the previous day and were re-exposed to the EPM. For each dose of CPA (8mg/kg and 16mg/kg) the animals were separated into four groups based on chronic treatment. In both experiments, the tests were recorded for the analysis of ethological measures and conventional measures [number of entries in open arms (OAE), enclosed (EAE) and total number of entries (TE), time spent in open arms (OAT), enclosed (EAT) and central area (CT), and their respective percentages]. Anxiety was assessed by the activity in the open arms (OA) in T1 (OAE, %OAE, OAT and %OAT), and decreased exploration of open arms on re-exposure was considered indicative of learning and memory. For data analysis, ANOVA (Two-way) followed by multiple comparison test Student-Newman-Keuls (SNK) (p <0.05) were used. The results of experiment 1 did not show difference between the groups in the variables related to exploration in the open arms (OAE, %OAE, OAT and %OAT). The control group SAL/SAL and the LH/CPA group had a significant reduction in these variables in T2, which was not observed in the group treated with LH/SAL. There was no significant change in locomotor activity in either group. The results of experiment 2 showed no significant difference between groups in variables related to anxiety, and there was no significant change in locomotor activity. Only the group treated exclusively with CPA (16mg/kg) showed significant reduction in measures OAE, %OAE, OAT and %OAT between test days (SNK <0.05). The results of experiment 1 indicated that the L-histidine caused a deficit in acquisition or recall of information of aversive open arms, and that chlorpheniramine was able to reverse this effect, suggesting the action of LH via the H1 receptor. The results of experiment 2 indicated that the chronic application of CPA did not affect the anxiety levels of mice exposed to the EPM and the information of aversive OA obtained in T1 was recalled only for animals treated exclusively with CPA (16mg/kg).
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spelling Gianlorenço, Anna Carolyna LepesteurMattioli, Rosanahttp://lattes.cnpq.br/5694498670428619http://lattes.cnpq.br/3861050459671690cf551ea9-6178-4f74-8348-a1d8411699bc2016-06-02T20:19:13Z2010-03-172016-06-02T20:19:13Z2010-02-26GIANLORENÇO, Anna Carolyna Lepesteur. Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado. 2010. 94 f. Dissertação (Mestrado em Ciências Biológicas) - Universidade Federal de São Carlos, São Carlos, 2010.https://repositorio.ufscar.br/handle/20.500.14289/5259The aim of this study was to assess the influence of histaminergic substances on anxiety and emotional memory in mice exposed and re-exposed to the Elevated Plus-Maze (EPM). For this, two experiments were conducted. Experiment 1 evaluated the effects of L-histidine on anxiety and emotional memory and contribution of the H 1 antagonist (chlorpheniramine) for these effects. Experiment 2 evaluated the effect of chronic treatment with chlorpheniramine (CPA) on anxiety and emotional memory. The experiments were performed with Swiss-albino mice (25-35g), using the model of the EPM in two consecutive days, exposure (T1) and reexposure (T2). In experiment 1, animals received combined intraperitoneal injection pretrial in T1: SAL/SAL (saline + saline), LH/SAL (L-histidine 500mg/kg + saline) and LH/CPA (Lhistidine + Chlorpheniramine 16mg/kg). The combined injection was executed by one first injection, followed by a second injection 30 minutes later. The test was performed in the EPM 10 minutes after the last injection. Each animal was positioned on the center platform of the maze facing the open arm and had five minutes to explore. After 24 hours (T2), the animals received the same pharmacological treatment of the previous day and were re-exposed to the EPM, following the procedures described. In experiment 2, the procedure was the application of chronic injections of SAL or CPA, intraperitoneally (i.p.) for 15 days. After this period, on the first day of test (T1), the animals were injected i.p. with SAL or CPA and 40 minutes later were exposed to EPM for 5 minutes. In T2, the animals received the same pharmacological treatment the previous day and were re-exposed to the EPM. For each dose of CPA (8mg/kg and 16mg/kg) the animals were separated into four groups based on chronic treatment. In both experiments, the tests were recorded for the analysis of ethological measures and conventional measures [number of entries in open arms (OAE), enclosed (EAE) and total number of entries (TE), time spent in open arms (OAT), enclosed (EAT) and central area (CT), and their respective percentages]. Anxiety was assessed by the activity in the open arms (OA) in T1 (OAE, %OAE, OAT and %OAT), and decreased exploration of open arms on re-exposure was considered indicative of learning and memory. For data analysis, ANOVA (Two-way) followed by multiple comparison test Student-Newman-Keuls (SNK) (p <0.05) were used. The results of experiment 1 did not show difference between the groups in the variables related to exploration in the open arms (OAE, %OAE, OAT and %OAT). The control group SAL/SAL and the LH/CPA group had a significant reduction in these variables in T2, which was not observed in the group treated with LH/SAL. There was no significant change in locomotor activity in either group. The results of experiment 2 showed no significant difference between groups in variables related to anxiety, and there was no significant change in locomotor activity. Only the group treated exclusively with CPA (16mg/kg) showed significant reduction in measures OAE, %OAE, OAT and %OAT between test days (SNK <0.05). The results of experiment 1 indicated that the L-histidine caused a deficit in acquisition or recall of information of aversive open arms, and that chlorpheniramine was able to reverse this effect, suggesting the action of LH via the H1 receptor. The results of experiment 2 indicated that the chronic application of CPA did not affect the anxiety levels of mice exposed to the EPM and the information of aversive OA obtained in T1 was recalled only for animals treated exclusively with CPA (16mg/kg).O objetivo desse estudo foi verificar a influência de substâncias histaminérgicas sobre a ansiedade e a memória emocional de camundongos expostos e reexpostos ao Labirinto em Cruz Elevado (LCE). Para isso, foram realizados dois experimentos. O experimento 1 avaliou os efeitos da L-histidina sobre a ansiedade e a memória emocional e a influência do antagonista H1 (Clorfeniramina) para esses efeitos. O experimento 2 avaliou o efeito do tratamento crônico com Clorfeniramina (CPA) sobre a ansiedade e a memória emocional. Os experimentos foram realizados com camundongos da cepa Suíço-albino (25-35g), utilizando o modelo do LCE em dois dias consecutivos, exposição (T1) e reexposição (T2). No experimento 1, os animais receberam injeção combinada, intraperitonealmente (i.p.), pré-teste em T1 de: SAL/SAL (salina+salina), LH/SAL (L-histidina 500mg/kg+salina) e LH/CPA (Lhistidina+ Clorfeniramina 16mg/kg). A injeção combinada consistiu na aplicação da primeira injeção, após 30 minutos uma segunda injeção, e depois de 10 minutos exposição ao LCE. Cada animal foi posicionado no centro do labirinto com a face voltada para o braço aberto e teve cinco minutos para exploração. Depois de 24 horas (T2), os animais receberam o mesmo tratamento farmacológico do dia anterior e foram reexpostos ao LCE, seguindo os procedimentos descritos. No experimento 2, o procedimento consistiu na aplicação de injeções crônicas de SAL ou CPA, i.p., por 15 dias. Após esse período, no primeiro dia de teste (T1), os animais receberam injeção i.p. de SAL ou CPA e 40 minutos depois foram expostos ao LCE por 5 minutos. Em T2, os animais receberam o mesmo tratamento farmacológico do dia anterior e foram reexpostos ao LCE. Para cada dose de CPA (8mg/kg e 16mg/kg) foi realizado um grupo controle. Nos dois experimentos, os testes foram gravados para a análise das medidas etológicas e espaço-temporais [número de entradas nos braços abertos (EBA), fechados (EBF) e número total de entradas (TE); tempo gasto nos braços abertos (TBA), fechados (TBF) e no centro (TC), e suas respectivas porcentagens]. A ansiedade foi avaliada pela atividade nos braços abertos (BA) em T1 (EBA, %EBA, TBA e %TBA), a diminuição da exploração dos braços abertos na reexposição foi considerada indicativo de aprendizagem e memória, e as EBF avaliaram a atividade locomotora. Para análise dos dados foi utilizada a ANOVA (Two-way) seguida pelo teste de comparações múltiplas Student-Newman-Keuls (SNK) (p<0,05). Os resultados do experimento 1 mostraram que nas variáveis referentes à exploração dos braços abertos (EBA, %EBA, TBA e %TBA) não houve diferença significativa entre os grupos em T1. O grupo controle SAL/SAL e o grupo LH/CPA apresentaram redução significativa dessas medidas em T2, o que não foi observado no grupo tratado com LH/SAL. Não houve alteração significativa na atividade locomotora em nenhum dos grupos. Os resultados do experimento 2 mostraram que não houve diferença significativa entre os grupos nas variáveis relativas à ansiedade, e que não houve alteração significativa na atividade locomotora. Somente o grupo tratado exclusivamente com CPA (16mg/kg) apresentou redução significativa nas medidas EBA, %EBA, TBA e %TBA entre os dias de teste (SNK<0,05). Os resultados do experimento 1 indicaram que a LH provocou um déficit na aquisição e/ou evocação da informação aversiva dos braços abertos, e que a Clorfeniramina foi capaz de reverter esse efeito, sugerindo ação da LH via receptor H1. Os resultados do experimento 2 indicaram que o tratamento crônico de CPA não alterou os níveis de ansiedade de camundongos expostos ao LCE e que a informação aversiva dos BA obtida em T1 foi evocada apenas pelos animais tratados exclusivamente com CPA (16mg/Kg).Universidade Federal de Minas Geraisapplication/pdfporUniversidade Federal de São CarlosPrograma de Pós-Graduação em Fisioterapia - PPGFtUFSCarBRAnsiedadeAprendizagem e memóriaL-HistidinaClorfeniraminaLabirinto em cruz elevadoCIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONALPapel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevadoinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesis5d090b7b-6f8c-4399-99cc-b6ed72e3bfbcinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFSCARinstname:Universidade Federal de São Carlos (UFSCAR)instacron:UFSCARTEXT2833.pdf.txt2833.pdf.txtExtracted texttext/plain102117https://repositorio.ufscar.br/bitstreams/a61685c7-9319-4732-848c-9145421cb31e/download54faa730d7fbc41651e24166b21689c3MD53falseAnonymousREADORIGINAL2833.pdfapplication/pdf1340809https://repositorio.ufscar.br/bitstreams/f958904f-cc5b-4289-a787-d6228f809fc6/downloadf1d7adcd72f8e79f64467c0eb7df287bMD51trueAnonymousREADTHUMBNAIL2833.pdf.jpg2833.pdf.jpgIM Thumbnailimage/jpeg7884https://repositorio.ufscar.br/bitstreams/84d199ad-e79b-4034-acf7-45360e6c348e/downloadd315834da3ea5e81ad95002ace62c4cbMD52falseAnonymousREAD20.500.14289/52592025-02-06 04:22:30.243open.accessoai:repositorio.ufscar.br:20.500.14289/5259https://repositorio.ufscar.brRepositório InstitucionalPUBhttps://repositorio.ufscar.br/oai/requestrepositorio.sibi@ufscar.bropendoar:43222025-02-06T07:22:30Repositório Institucional da UFSCAR - Universidade Federal de São Carlos (UFSCAR)false
dc.title.por.fl_str_mv Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
title Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
spellingShingle Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
Gianlorenço, Anna Carolyna Lepesteur
Ansiedade
Aprendizagem e memória
L-Histidina
Clorfeniramina
Labirinto em cruz elevado
CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL
title_short Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
title_full Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
title_fullStr Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
title_full_unstemmed Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
title_sort Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado
author Gianlorenço, Anna Carolyna Lepesteur
author_facet Gianlorenço, Anna Carolyna Lepesteur
author_role author
dc.contributor.authorlattes.por.fl_str_mv http://lattes.cnpq.br/3861050459671690
dc.contributor.author.fl_str_mv Gianlorenço, Anna Carolyna Lepesteur
dc.contributor.advisor1.fl_str_mv Mattioli, Rosana
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/5694498670428619
dc.contributor.authorID.fl_str_mv cf551ea9-6178-4f74-8348-a1d8411699bc
contributor_str_mv Mattioli, Rosana
dc.subject.por.fl_str_mv Ansiedade
Aprendizagem e memória
L-Histidina
Clorfeniramina
Labirinto em cruz elevado
topic Ansiedade
Aprendizagem e memória
L-Histidina
Clorfeniramina
Labirinto em cruz elevado
CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL
dc.subject.cnpq.fl_str_mv CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL
description The aim of this study was to assess the influence of histaminergic substances on anxiety and emotional memory in mice exposed and re-exposed to the Elevated Plus-Maze (EPM). For this, two experiments were conducted. Experiment 1 evaluated the effects of L-histidine on anxiety and emotional memory and contribution of the H 1 antagonist (chlorpheniramine) for these effects. Experiment 2 evaluated the effect of chronic treatment with chlorpheniramine (CPA) on anxiety and emotional memory. The experiments were performed with Swiss-albino mice (25-35g), using the model of the EPM in two consecutive days, exposure (T1) and reexposure (T2). In experiment 1, animals received combined intraperitoneal injection pretrial in T1: SAL/SAL (saline + saline), LH/SAL (L-histidine 500mg/kg + saline) and LH/CPA (Lhistidine + Chlorpheniramine 16mg/kg). The combined injection was executed by one first injection, followed by a second injection 30 minutes later. The test was performed in the EPM 10 minutes after the last injection. Each animal was positioned on the center platform of the maze facing the open arm and had five minutes to explore. After 24 hours (T2), the animals received the same pharmacological treatment of the previous day and were re-exposed to the EPM, following the procedures described. In experiment 2, the procedure was the application of chronic injections of SAL or CPA, intraperitoneally (i.p.) for 15 days. After this period, on the first day of test (T1), the animals were injected i.p. with SAL or CPA and 40 minutes later were exposed to EPM for 5 minutes. In T2, the animals received the same pharmacological treatment the previous day and were re-exposed to the EPM. For each dose of CPA (8mg/kg and 16mg/kg) the animals were separated into four groups based on chronic treatment. In both experiments, the tests were recorded for the analysis of ethological measures and conventional measures [number of entries in open arms (OAE), enclosed (EAE) and total number of entries (TE), time spent in open arms (OAT), enclosed (EAT) and central area (CT), and their respective percentages]. Anxiety was assessed by the activity in the open arms (OA) in T1 (OAE, %OAE, OAT and %OAT), and decreased exploration of open arms on re-exposure was considered indicative of learning and memory. For data analysis, ANOVA (Two-way) followed by multiple comparison test Student-Newman-Keuls (SNK) (p <0.05) were used. The results of experiment 1 did not show difference between the groups in the variables related to exploration in the open arms (OAE, %OAE, OAT and %OAT). The control group SAL/SAL and the LH/CPA group had a significant reduction in these variables in T2, which was not observed in the group treated with LH/SAL. There was no significant change in locomotor activity in either group. The results of experiment 2 showed no significant difference between groups in variables related to anxiety, and there was no significant change in locomotor activity. Only the group treated exclusively with CPA (16mg/kg) showed significant reduction in measures OAE, %OAE, OAT and %OAT between test days (SNK <0.05). The results of experiment 1 indicated that the L-histidine caused a deficit in acquisition or recall of information of aversive open arms, and that chlorpheniramine was able to reverse this effect, suggesting the action of LH via the H1 receptor. The results of experiment 2 indicated that the chronic application of CPA did not affect the anxiety levels of mice exposed to the EPM and the information of aversive OA obtained in T1 was recalled only for animals treated exclusively with CPA (16mg/kg).
publishDate 2010
dc.date.available.fl_str_mv 2010-03-17
2016-06-02T20:19:13Z
dc.date.issued.fl_str_mv 2010-02-26
dc.date.accessioned.fl_str_mv 2016-06-02T20:19:13Z
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dc.identifier.citation.fl_str_mv GIANLORENÇO, Anna Carolyna Lepesteur. Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado. 2010. 94 f. Dissertação (Mestrado em Ciências Biológicas) - Universidade Federal de São Carlos, São Carlos, 2010.
dc.identifier.uri.fl_str_mv https://repositorio.ufscar.br/handle/20.500.14289/5259
identifier_str_mv GIANLORENÇO, Anna Carolyna Lepesteur. Papel do sistema histaminérgico na memória emocional de camundongos expostos e reexpostos ao labirinto em cruz elevado. 2010. 94 f. Dissertação (Mestrado em Ciências Biológicas) - Universidade Federal de São Carlos, São Carlos, 2010.
url https://repositorio.ufscar.br/handle/20.500.14289/5259
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