Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas

Detalhes bibliográficos
Ano de defesa: 2019
Autor(a) principal: Raimundo, Breno Vilas Boas lattes
Orientador(a): Castro, Lívia De Figueiredo Diniz lattes
Banca de defesa: Francisco, Amanda Fortes, Caldas, Sérgio
Tipo de documento: Dissertação
Tipo de acesso: Acesso aberto
Idioma: por
Instituição de defesa: Universidade Federal de Alfenas
Programa de Pós-Graduação: Programa de Pós-graduação em Ciências Biológicas
Departamento: Instituto de Ciências da Natureza
País: Brasil
Palavras-chave em Português:
Antifúngicos
Amiodarona
Trypanosoma cruzi
Área do conhecimento CNPq:
PARASITOLOGIA::PROTOZOOLOGIA DE PARASITOS
Link de acesso: https://repositorio.unifal-mg.edu.br/handle/123456789/1717
Resumo: Although many advances have been made in the field of Chagas disease chemotherapy in recent years, there is still no treatment with a satisfactory efficacy and safety profile for the chronic phase of Trypanosoma cruzi infection. Repositioning and drug combination have been highlighted as promising strategies in the search for new therapies. However, in parallel with the search for new alternatives, it is necessary to improve existing preclinical evaluation models. In this sense, the aim of the present study was to evaluate the effects of ravuconazole in combination with amiodarone on the development of acute T. cruzi infection in different experimental models. Initially, in vitro experiments were performed to determine the toxicity of the combination and the nature of the drugs on the infection of H9c2 cells by Y strain of T. cruzi. Subsequently, in vivo experiments were performed using different lineages of mice (Swiss and BALB/c) and strains of the parasite that show varying degrees of resistance to etiological treatment (Y and Colombian). The infected animals were treated from the 5th (strain Y) or 10th (Colombian strain) day after infection for 5 days orally with ravuconazole (0.5mg/kg) and amiodarone (50mg/kg) alone and in combination. Uninfected control group, infected and untreated group, infected and treated with ravuconazole at 10mg/kg or benznidazole at the dose of 100mg / kg were also included. The parasitemia was quantified daily during the whole period of the experiment. Five days after the end of treatment the animals were euthanized and the heart collected for histological analysis. The obtained results allowed to confirm the trypanosomicidal activity of the drugs and to identify additive effect resulting from the combination between amiodarone and ravuconazole in vitro, in the absence of additional toxicity. In vivo, amiodarone was not efficient in controlling infection by different strains of the parasite, whereas the effect of ravuconazole on Y strain was dependent on the dose and mouse strain used; while at 10 mg/kg azole suppressed the parasitemia of Y strain infected animals in both strains, the effect of underdose on parasitism control was significantly lower in BALB/c. On the other hand, combined therapy was effective in reducing the area under the parasitemia curve compared to monotherapies, regardless of mouse strain, suggesting a positive interaction between drugs. Interestingly, ravuconazole underdose drastically reduced parasitemia in mice infected with the Colombian strain while the combination did not induce additional benefit. Histopathological evaluation of cardiac muscle tissue showed that the combined use of ravuconazole and amiodarone, unlike monotherapy at the same doses, mitigated the damage caused by infection, regardless of the parasite strain or host lineage. The data obtained allow to conclude that the experimental strategy adopted was efficient to evaluate the interaction between drugs and suggest that the BALB/c lineage is a more stringent model for preclinical studies in Chagas disease chemotherapy. In addition, ravuconazole and amiodarone combined have a superior effect than monotherapies in reducing parasitism and preventing heart damage due to infection.
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spelling Raimundo, Breno Vilas Boashttp://lattes.cnpq.br/0683364443442719Silva, Ana Lia MazzetiFrancisco, Amanda FortesCaldas, SérgioCastro, Lívia De Figueiredo Dinizhttp://lattes.cnpq.br/46598180634549862021-02-04T13:47:08Z2019-12-16RAIMUNDO, Breno Vilas Boas. Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas. 2019. 82 f. Dissertação (Mestrado em Ciências Biológicas) - Universidade Federal de Alfenas, Alfenas, MG, 2019.https://repositorio.unifal-mg.edu.br/handle/123456789/1717Although many advances have been made in the field of Chagas disease chemotherapy in recent years, there is still no treatment with a satisfactory efficacy and safety profile for the chronic phase of Trypanosoma cruzi infection. Repositioning and drug combination have been highlighted as promising strategies in the search for new therapies. However, in parallel with the search for new alternatives, it is necessary to improve existing preclinical evaluation models. In this sense, the aim of the present study was to evaluate the effects of ravuconazole in combination with amiodarone on the development of acute T. cruzi infection in different experimental models. Initially, in vitro experiments were performed to determine the toxicity of the combination and the nature of the drugs on the infection of H9c2 cells by Y strain of T. cruzi. Subsequently, in vivo experiments were performed using different lineages of mice (Swiss and BALB/c) and strains of the parasite that show varying degrees of resistance to etiological treatment (Y and Colombian). The infected animals were treated from the 5th (strain Y) or 10th (Colombian strain) day after infection for 5 days orally with ravuconazole (0.5mg/kg) and amiodarone (50mg/kg) alone and in combination. Uninfected control group, infected and untreated group, infected and treated with ravuconazole at 10mg/kg or benznidazole at the dose of 100mg / kg were also included. The parasitemia was quantified daily during the whole period of the experiment. Five days after the end of treatment the animals were euthanized and the heart collected for histological analysis. The obtained results allowed to confirm the trypanosomicidal activity of the drugs and to identify additive effect resulting from the combination between amiodarone and ravuconazole in vitro, in the absence of additional toxicity. In vivo, amiodarone was not efficient in controlling infection by different strains of the parasite, whereas the effect of ravuconazole on Y strain was dependent on the dose and mouse strain used; while at 10 mg/kg azole suppressed the parasitemia of Y strain infected animals in both strains, the effect of underdose on parasitism control was significantly lower in BALB/c. On the other hand, combined therapy was effective in reducing the area under the parasitemia curve compared to monotherapies, regardless of mouse strain, suggesting a positive interaction between drugs. Interestingly, ravuconazole underdose drastically reduced parasitemia in mice infected with the Colombian strain while the combination did not induce additional benefit. Histopathological evaluation of cardiac muscle tissue showed that the combined use of ravuconazole and amiodarone, unlike monotherapy at the same doses, mitigated the damage caused by infection, regardless of the parasite strain or host lineage. The data obtained allow to conclude that the experimental strategy adopted was efficient to evaluate the interaction between drugs and suggest that the BALB/c lineage is a more stringent model for preclinical studies in Chagas disease chemotherapy. In addition, ravuconazole and amiodarone combined have a superior effect than monotherapies in reducing parasitism and preventing heart damage due to infection.Embora muitos avanços tenham sido realizados no âmbito da quimioterapia da doença de Chagas nos últimos anos, ainda não há tratamento com perfil satisfatório de eficácia e segurança para a fase crônica da infecção por Trypanosoma cruzi. O reposicionamento e a combinação de medicamentos têm se destacado como estratégias promissoras na busca de novas terapias. No entanto, paralelamente à busca por novas alternativas, é necessário aprimorar os modelos de avaliação pré-clínica existentes. Nesse sentido, o objetivo do presente estudo foi avaliar os efeitos do ravuconazol em combinação com amiodarona sobre o desenvolvimento da infecção aguda por T. cruzi em diferentes modelos experimentais. Inicialmente foram realizados experimentos in vitro para determinar a toxicidade da combinação e a natureza da interação entre os fármacos sobre a infecção de células H9c2 pela cepa Y de T. cruzi. Posteriormente foram realizados experimentos in vivo utilizando diferentes linhagens de camundongos (Swiss e BALB/c) e cepas do parasito que apresentam graus variáveis de resistência ao tratamento etiológico (Y e Colombiana). Os animais infectados foram tratados a partir do 5o (cepa Y) ou 10o (cepa Colombiana) dia após a infecção durante 5 dias, por via oral, com ravuconazol (0,5mg/Kg) e amiodarona (50mg/Kg) em monoterapia e em combinação. Grupos controle contendo animais não infectados, infectados e não tratados, infectados e tratados com ravuconazol a 10mg/Kg ou benznidazol na dose de 100mg/Kg foram também incluídos. A parasitemia foi quantificada diariamente durante todo o período de realização do experimento. Cinco dias após o término do tratamento os animais foram eutanasiados e o coração coletado para análises histológicas. Os resultados obtidos permitiram confirmar a atividade tripanossomicida dos fármacos e identificar efeito aditivo resultante da combinação entre amiodarona e ravuconazol in vitro, na ausência de toxicidade adicional. In vivo, a amiodarona não foi eficiente em controlar a infecção pelas diferentes cepas do parasito, já o efeito do ravuconazol sobre a cepa Y foi dependente da dose e da linhagem de camundongo utilizada; enquanto a 10 mg/Kg o azólico suprimiu a parasitemia dos animais infectados pela cepa Y em ambas as linhagens, o efeito da subdose em controlar o parasitismo foi significativamente menor nos BALB/c. Por outro lado, a terapia combinada foi efetiva em reduzir a área sob a curva de parasitemia comparativamente às monoterapias, independente da linhagem de camundongo, sugerindo interação positiva entre os fármacos. Curiosamente, o ravuconazol em subdose reduziu drasticamente a parasitemia dos camundongos infectados pela cepa Colombiana enquanto a combinação não induziu benefício adicional. A avaliação histopatológica do tecido muscular cardíaco mostrou que a utilização combinada de ravuconazol e amiodarona, ao contrário das monoterapias nas mesmas doses, amenizou os danos provocados pela infecção, independente da cepa do parasito ou da linhagem do hospedeiro. Os dados obtidos permitem concluir que a estratégia experimental adotada foi eficiente para avaliar a interação entre os fármacos e sugerem que a linhagem BALB/c constitui um modelo mais estringente para estudos pré-clínicos na quimioterapia da doença de Chagas. Ainda, o ravuconazol e amiodarona combinados apresentam efeito superior às monoterapias em reduzir o parasitismo e prevenir as lesões cardíacas decorrentes da infecção.Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPESapplication/pdfporUniversidade Federal de AlfenasPrograma de Pós-graduação em Ciências BiológicasUNIFAL-MGBrasilInstituto de Ciências da Naturezainfo:eu-repo/semantics/openAccesshttp://creativecommons.org/licenses/by-nc-nd/4.0/AntifúngicosAmiodaronaTrypanosoma cruziPARASITOLOGIA::PROTOZOOLOGIA DE PARASITOSEstudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagasinfo:eu-repo/semantics/masterThesisinfo:eu-repo/semantics/publishedVersion454226360311113921060060060028784769405680317212075167498588264571reponame:Repositório Institucional da Universidade Federal de Alfenas - RiUnifalinstname:Universidade Federal de Alfenas (UNIFAL)instacron:UNIFALRaimundo, Breno Vilas BoasLICENSElicense.txtlicense.txttext/plain; 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dc.title.pt-BR.fl_str_mv Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
title Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
spellingShingle Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
Raimundo, Breno Vilas Boas
Antifúngicos
Amiodarona
Trypanosoma cruzi
PARASITOLOGIA::PROTOZOOLOGIA DE PARASITOS
title_short Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
title_full Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
title_fullStr Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
title_full_unstemmed Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
title_sort Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas
author Raimundo, Breno Vilas Boas
author_facet Raimundo, Breno Vilas Boas
author_role author
dc.contributor.author.fl_str_mv Raimundo, Breno Vilas Boas
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/0683364443442719
dc.contributor.advisor-co1.fl_str_mv Silva, Ana Lia Mazzeti
dc.contributor.referee1.fl_str_mv Francisco, Amanda Fortes
dc.contributor.referee2.fl_str_mv Caldas, Sérgio
dc.contributor.advisor1.fl_str_mv Castro, Lívia De Figueiredo Diniz
dc.contributor.authorLattes.fl_str_mv http://lattes.cnpq.br/4659818063454986
contributor_str_mv Silva, Ana Lia Mazzeti
Francisco, Amanda Fortes
Caldas, Sérgio
Castro, Lívia De Figueiredo Diniz
dc.subject.por.fl_str_mv Antifúngicos
Amiodarona
Trypanosoma cruzi
topic Antifúngicos
Amiodarona
Trypanosoma cruzi
PARASITOLOGIA::PROTOZOOLOGIA DE PARASITOS
dc.subject.cnpq.fl_str_mv PARASITOLOGIA::PROTOZOOLOGIA DE PARASITOS
description Although many advances have been made in the field of Chagas disease chemotherapy in recent years, there is still no treatment with a satisfactory efficacy and safety profile for the chronic phase of Trypanosoma cruzi infection. Repositioning and drug combination have been highlighted as promising strategies in the search for new therapies. However, in parallel with the search for new alternatives, it is necessary to improve existing preclinical evaluation models. In this sense, the aim of the present study was to evaluate the effects of ravuconazole in combination with amiodarone on the development of acute T. cruzi infection in different experimental models. Initially, in vitro experiments were performed to determine the toxicity of the combination and the nature of the drugs on the infection of H9c2 cells by Y strain of T. cruzi. Subsequently, in vivo experiments were performed using different lineages of mice (Swiss and BALB/c) and strains of the parasite that show varying degrees of resistance to etiological treatment (Y and Colombian). The infected animals were treated from the 5th (strain Y) or 10th (Colombian strain) day after infection for 5 days orally with ravuconazole (0.5mg/kg) and amiodarone (50mg/kg) alone and in combination. Uninfected control group, infected and untreated group, infected and treated with ravuconazole at 10mg/kg or benznidazole at the dose of 100mg / kg were also included. The parasitemia was quantified daily during the whole period of the experiment. Five days after the end of treatment the animals were euthanized and the heart collected for histological analysis. The obtained results allowed to confirm the trypanosomicidal activity of the drugs and to identify additive effect resulting from the combination between amiodarone and ravuconazole in vitro, in the absence of additional toxicity. In vivo, amiodarone was not efficient in controlling infection by different strains of the parasite, whereas the effect of ravuconazole on Y strain was dependent on the dose and mouse strain used; while at 10 mg/kg azole suppressed the parasitemia of Y strain infected animals in both strains, the effect of underdose on parasitism control was significantly lower in BALB/c. On the other hand, combined therapy was effective in reducing the area under the parasitemia curve compared to monotherapies, regardless of mouse strain, suggesting a positive interaction between drugs. Interestingly, ravuconazole underdose drastically reduced parasitemia in mice infected with the Colombian strain while the combination did not induce additional benefit. Histopathological evaluation of cardiac muscle tissue showed that the combined use of ravuconazole and amiodarone, unlike monotherapy at the same doses, mitigated the damage caused by infection, regardless of the parasite strain or host lineage. The data obtained allow to conclude that the experimental strategy adopted was efficient to evaluate the interaction between drugs and suggest that the BALB/c lineage is a more stringent model for preclinical studies in Chagas disease chemotherapy. In addition, ravuconazole and amiodarone combined have a superior effect than monotherapies in reducing parasitism and preventing heart damage due to infection.
publishDate 2019
dc.date.issued.fl_str_mv 2019-12-16
dc.date.accessioned.fl_str_mv 2021-02-04T13:47:08Z
dc.type.driver.fl_str_mv info:eu-repo/semantics/masterThesis
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
format masterThesis
status_str publishedVersion
dc.identifier.citation.fl_str_mv RAIMUNDO, Breno Vilas Boas. Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas. 2019. 82 f. Dissertação (Mestrado em Ciências Biológicas) - Universidade Federal de Alfenas, Alfenas, MG, 2019.
dc.identifier.uri.fl_str_mv https://repositorio.unifal-mg.edu.br/handle/123456789/1717
identifier_str_mv RAIMUNDO, Breno Vilas Boas. Estudo de modelos experimentais aplicáveis à seleção de combinações de fármacos em avaliações pré-clínicas da doença de chagas. 2019. 82 f. Dissertação (Mestrado em Ciências Biológicas) - Universidade Federal de Alfenas, Alfenas, MG, 2019.
url https://repositorio.unifal-mg.edu.br/handle/123456789/1717
dc.language.iso.fl_str_mv por
language por
dc.relation.department.fl_str_mv 4542263603111139210
dc.relation.confidence.fl_str_mv 600
600
600
dc.relation.cnpq.fl_str_mv 2878476940568031721
dc.relation.sponsorship.fl_str_mv 2075167498588264571
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
http://creativecommons.org/licenses/by-nc-nd/4.0/
eu_rights_str_mv openAccess
rights_invalid_str_mv http://creativecommons.org/licenses/by-nc-nd/4.0/
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dc.publisher.none.fl_str_mv Universidade Federal de Alfenas
dc.publisher.program.fl_str_mv Programa de Pós-graduação em Ciências Biológicas
dc.publisher.initials.fl_str_mv UNIFAL-MG
dc.publisher.country.fl_str_mv Brasil
dc.publisher.department.fl_str_mv Instituto de Ciências da Natureza
publisher.none.fl_str_mv Universidade Federal de Alfenas
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repository.name.fl_str_mv Repositório Institucional da Universidade Federal de Alfenas - RiUnifal - Universidade Federal de Alfenas (UNIFAL)
repository.mail.fl_str_mv repositorio@unifal-mg.edu.br
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