Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo

Detalhes bibliográficos
Autor(a) principal: Sperotto , Nathalia Denise de Moura
Data de Publicação: 2020
Tipo de documento: Tese
Idioma: por
Título da fonte: Biblioteca Digital de Teses e Dissertações da PUC_RS
Texto Completo: http://tede2.pucrs.br/tede2/handle/tede/9289
Resumo: Human thymidine phosphorylase (hTP) is an enzyme responsible for catalizing the phosphorolysis of thymidine in thymine and 2-deoxy-D-ribose-1-phosphate, being overexpressed in several solid tumors, including glioblastoma and colorectal carcinoma. The present study aimed to investigate the toxicological and pharmacological profiles of CPBMF-223 compound - a potent noncompetitive hTP inhibitor -, in a glioblastoma and colorectal carcinoma animal models. To evaluate the toxicity of CPBMF-223, in vitro assays of cytotoxicity (25 – 1000 μM), genotoxicity (250 – 1000 μM) and mutagenesis (100 – 2000 μg/plate) were performed. In addition, the cardiotoxicity and neurotoxicity effects were assessed in zebrafish larvae (50 – 500 μM), as well as the acute oral toxicity in mice (300 and 2000 mg/kg). The pharmacokinetic profile of the hTP inhibitor was analysed by intravenous (i.v.), intraperitoneal (i.p.), and oral as well as the plasma protein binding capacity. The pharmacological effects of CPBMF-223 (50 mg/kg, 5 days/week) were observed on the tumor growth in the xenographic model induced by human glioblastoma cells (U-87 MG) and human colorectal cancer (HCT-116) in nude mice (female and male). Interestingly, the results showed that CPBMF-223 did not induce cytotoxicity, genotoxicity and mutagenic effects. Moreveover, no significant changes was noted in acute toxicity experiments, with a slightly low toxic profile in the zebrafish model. CPBMF-223 also demonstrated a high bioavailaibity (>100%) in i.p. administration and low plasma protein binding (34%). Notably, the hTP inhibitor was able to reduce the relative tumor volume and the tumor growth rate, in both experimental models. In the glioblastoma model, the inhibition rate was 31% in male mice, and 50% in the colorectal model. For female, the percentage of reduction was 50% in the colorectal model. Interestingly, in both in vivo models, CPBMF-223 was able to decrease the tumors number of blood vesses and did not modify the liver injury enzymes. Collectively, the resuts bring new evidence of the toxicological safety of the CPBMF-223 compound and the antitumor activity performed in in vivo cancer models, pointing out this inhibitor as a promising drug to cancer treatment.
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spelling Basso , Luiz Augustohttp://lattes.cnpq.br/3431777523511296Rodrigues Junior , Valnês da Silvahttp://lattes.cnpq.br/6489536459329379http://lattes.cnpq.br/0191942878266069Sperotto , Nathalia Denise de Moura2020-10-26T19:53:44Z2020-03-27http://tede2.pucrs.br/tede2/handle/tede/9289Human thymidine phosphorylase (hTP) is an enzyme responsible for catalizing the phosphorolysis of thymidine in thymine and 2-deoxy-D-ribose-1-phosphate, being overexpressed in several solid tumors, including glioblastoma and colorectal carcinoma. The present study aimed to investigate the toxicological and pharmacological profiles of CPBMF-223 compound - a potent noncompetitive hTP inhibitor -, in a glioblastoma and colorectal carcinoma animal models. To evaluate the toxicity of CPBMF-223, in vitro assays of cytotoxicity (25 – 1000 μM), genotoxicity (250 – 1000 μM) and mutagenesis (100 – 2000 μg/plate) were performed. In addition, the cardiotoxicity and neurotoxicity effects were assessed in zebrafish larvae (50 – 500 μM), as well as the acute oral toxicity in mice (300 and 2000 mg/kg). The pharmacokinetic profile of the hTP inhibitor was analysed by intravenous (i.v.), intraperitoneal (i.p.), and oral as well as the plasma protein binding capacity. The pharmacological effects of CPBMF-223 (50 mg/kg, 5 days/week) were observed on the tumor growth in the xenographic model induced by human glioblastoma cells (U-87 MG) and human colorectal cancer (HCT-116) in nude mice (female and male). Interestingly, the results showed that CPBMF-223 did not induce cytotoxicity, genotoxicity and mutagenic effects. Moreveover, no significant changes was noted in acute toxicity experiments, with a slightly low toxic profile in the zebrafish model. CPBMF-223 also demonstrated a high bioavailaibity (>100%) in i.p. administration and low plasma protein binding (34%). Notably, the hTP inhibitor was able to reduce the relative tumor volume and the tumor growth rate, in both experimental models. In the glioblastoma model, the inhibition rate was 31% in male mice, and 50% in the colorectal model. For female, the percentage of reduction was 50% in the colorectal model. Interestingly, in both in vivo models, CPBMF-223 was able to decrease the tumors number of blood vesses and did not modify the liver injury enzymes. Collectively, the resuts bring new evidence of the toxicological safety of the CPBMF-223 compound and the antitumor activity performed in in vivo cancer models, pointing out this inhibitor as a promising drug to cancer treatment.A timidina fosforilase humana (hTP) é uma enzima responsável por catalisar a fosforólise de timidina em timina e 2-deoxi-D-ribose-1-fosfato, sendo altamente expressa em diversos tumores sólidos, incluindo glioblastoma e carcinoma colorretal. O presente trabalho teve como objetivo investigar o perfil toxicológico e farmacológico do composto CPBMF-223 – um potente inibidor não competitivo da hTP –, em modelo animal de glioblastoma e de carcinoma colorretal. Para a avaliação da toxicidade do CPBMF-223, foram realizados estudos in vitro de citotoxicidade (25 - 1000 μM), genotoxicidade (250 - 1000 μM) e mutagênese (100 - 2000 μg/placa). Além disso, foram investigados os efeitos em parâmetros de cardiotoxicidade e neurotoxicidade em larvas de peixe-zebra (50 - 500 μM), assim como no ensaio de toxicidade oral em camundongos (300 e 2000 mg/kg). O perfil farmacocinético do inibidor da hTP foi analisado pelas vias intravenosa (i.v.), intraperitoneal (i.p.) e oral, bem como a capacidade de ligação a proteína plasmática. Os efeitos farmacológicos do CPBMF-223, (50 mg/kg/dia, 5 dias/semana) foram obervados sobre o crescimento tumoral no modelo xenográficos induzido por células humanas de glioblastoma (U-87 MG) e de câncer de colorretal (HCT-116) em camundongos nude (machos e fêmeas). De maneira interessante, os resultados mostram que o CPBMF-223 não induziu citotoxicidade, além de não apresentar efeitos genotóxicos e mutagênicos. Não foi observado alterações significativas na toxicidade aguda em roedores, e mostrou baixo perfil tóxico em modelo de peixe-zebra. O CPBMF-223 demonstrou uma alta biodisponibilidade (>100%) quando administrado pela via i.p., e baixa ligação a proteína plasmática (34%). Notavelmente, o inibidor da hTP foi capaz de reduzir o volume relativo do tumor e a taxa de crescimento tumoral, em ambos os modelos experimentais. No modelo de glioblastoma, a taxa de inibição foi de 31% em camundongos machos, e de 50% no modelo experimental de colorretal. Para as fêmeas, houve uma redução de 50% no modelo in vivo de câncer de colorretal. Interessantemente, em ambos os modelos animais, o CPBMF-223 foi capaz de diminuir o número de vasos sanguíneos presente nos tumores e não modificou enzimas preditoras de lesão hepática. Coletivamente, os resultados trazem novas evidências da segurança toxicológica do composto CPBMF-223 e da atividade antitumoral desempenhada em modelos in vivo de câncer, apontando esse inibidor como um promissor fármaco no tratamento de cânceres.Submitted by PPG Medicina e Ciências da Saúde (medicina-pg@pucrs.br) on 2020-07-24T14:00:14Z No. of bitstreams: 1 Tese Nathalia Sperotto 2020.pdf: 20091595 bytes, checksum: f680471ab963a6c83d03895b41bd1f09 (MD5)Approved for entry into archive by Clarissa Selbach (clarissa.selbach@pucrs.br) on 2020-10-26T19:49:15Z (GMT) No. of bitstreams: 1 Tese Nathalia Sperotto 2020.pdf: 20091595 bytes, checksum: f680471ab963a6c83d03895b41bd1f09 (MD5)Made available in DSpace on 2020-10-26T19:53:44Z (GMT). No. of bitstreams: 1 Tese Nathalia Sperotto 2020.pdf: 20091595 bytes, checksum: f680471ab963a6c83d03895b41bd1f09 (MD5) Previous issue date: 2020-03-27Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPESapplication/pdfhttp://tede2.pucrs.br:80/tede2/retrieve/179130/TES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.jpgporPontifícia Universidade Católica do Rio Grande do SulPrograma de Pós-Graduação em Medicina e Ciências da SaúdePUCRSBrasilEscola de MedicinaTimidina fosforilase humanaCPBMF-223GlioblastomaCâncer colorretalCamundongos nudeModelo xenográficoHuman thymidine phophorylaseCPBMF-223GlioblastomaColorectal cancerNude miceXenogaft cancer modelCIENCIAS DA SAUDE::MEDICINAAvaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivoinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesisTrabalho será publicado como artigo ou livro60 meses26/10/2025-721401722658532398500500500600-224747486637135387-9693694523087866273590462550136975366info:eu-repo/semantics/openAccessreponame:Biblioteca Digital de Teses e Dissertações da PUC_RSinstname:Pontifícia Universidade Católica do Rio Grande do Sul (PUCRS)instacron:PUC_RSTHUMBNAILTES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.jpgTES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.jpgimage/jpeg4103http://tede2.pucrs.br/tede2/bitstream/tede/9289/4/TES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.jpg60bfbfc76e788d4da9e9d9713f40a81aMD54TEXTTES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.txtTES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.txttext/plain2015http://tede2.pucrs.br/tede2/bitstream/tede/9289/3/TES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdf.txt2639a093141a89b6ba19fa912281a95aMD53ORIGINALTES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdfTES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdfapplication/pdf449650http://tede2.pucrs.br/tede2/bitstream/tede/9289/2/TES_NATHALIA_DENISE_DE_MOURA_SPEROTTO_CONFIDENCIAL.pdfa465d3fe4fb8f962ec0fc154386d45cfMD52LICENSElicense.txtlicense.txttext/plain; charset=utf-8590http://tede2.pucrs.br/tede2/bitstream/tede/9289/1/license.txt220e11f2d3ba5354f917c7035aadef24MD51tede/92892020-10-26 21:00:09.11oai:tede2.pucrs.br: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Biblioteca Digital de Teses e Dissertaçõeshttp://tede2.pucrs.br/tede2/PRIhttps://tede2.pucrs.br/oai/requestbiblioteca.central@pucrs.br||opendoar:2020-10-26T23:00:09Biblioteca Digital de Teses e Dissertações da PUC_RS - Pontifícia Universidade Católica do Rio Grande do Sul (PUCRS)false
dc.title.por.fl_str_mv Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
title Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
spellingShingle Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
Sperotto , Nathalia Denise de Moura
Timidina fosforilase humana
CPBMF-223
Glioblastoma
Câncer colorretal
Camundongos nude
Modelo xenográfico
Human thymidine phophorylase
CPBMF-223
Glioblastoma
Colorectal cancer
Nude mice
Xenogaft cancer model
CIENCIAS DA SAUDE::MEDICINA
title_short Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
title_full Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
title_fullStr Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
title_full_unstemmed Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
title_sort Avaliação da atividade antitumoral e do perfil toxicológico do composto CPBMF-223 em experimentos in vitro e in vivo
author Sperotto , Nathalia Denise de Moura
author_facet Sperotto , Nathalia Denise de Moura
author_role author
dc.contributor.advisor1.fl_str_mv Basso , Luiz Augusto
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/3431777523511296
dc.contributor.advisor-co1.fl_str_mv Rodrigues Junior , Valnês da Silva
dc.contributor.advisor-co1Lattes.fl_str_mv http://lattes.cnpq.br/6489536459329379
dc.contributor.authorLattes.fl_str_mv http://lattes.cnpq.br/0191942878266069
dc.contributor.author.fl_str_mv Sperotto , Nathalia Denise de Moura
contributor_str_mv Basso , Luiz Augusto
Rodrigues Junior , Valnês da Silva
dc.subject.por.fl_str_mv Timidina fosforilase humana
CPBMF-223
Glioblastoma
Câncer colorretal
Camundongos nude
Modelo xenográfico
topic Timidina fosforilase humana
CPBMF-223
Glioblastoma
Câncer colorretal
Camundongos nude
Modelo xenográfico
Human thymidine phophorylase
CPBMF-223
Glioblastoma
Colorectal cancer
Nude mice
Xenogaft cancer model
CIENCIAS DA SAUDE::MEDICINA
dc.subject.eng.fl_str_mv Human thymidine phophorylase
CPBMF-223
Glioblastoma
Colorectal cancer
Nude mice
Xenogaft cancer model
dc.subject.cnpq.fl_str_mv CIENCIAS DA SAUDE::MEDICINA
description Human thymidine phosphorylase (hTP) is an enzyme responsible for catalizing the phosphorolysis of thymidine in thymine and 2-deoxy-D-ribose-1-phosphate, being overexpressed in several solid tumors, including glioblastoma and colorectal carcinoma. The present study aimed to investigate the toxicological and pharmacological profiles of CPBMF-223 compound - a potent noncompetitive hTP inhibitor -, in a glioblastoma and colorectal carcinoma animal models. To evaluate the toxicity of CPBMF-223, in vitro assays of cytotoxicity (25 – 1000 μM), genotoxicity (250 – 1000 μM) and mutagenesis (100 – 2000 μg/plate) were performed. In addition, the cardiotoxicity and neurotoxicity effects were assessed in zebrafish larvae (50 – 500 μM), as well as the acute oral toxicity in mice (300 and 2000 mg/kg). The pharmacokinetic profile of the hTP inhibitor was analysed by intravenous (i.v.), intraperitoneal (i.p.), and oral as well as the plasma protein binding capacity. The pharmacological effects of CPBMF-223 (50 mg/kg, 5 days/week) were observed on the tumor growth in the xenographic model induced by human glioblastoma cells (U-87 MG) and human colorectal cancer (HCT-116) in nude mice (female and male). Interestingly, the results showed that CPBMF-223 did not induce cytotoxicity, genotoxicity and mutagenic effects. Moreveover, no significant changes was noted in acute toxicity experiments, with a slightly low toxic profile in the zebrafish model. CPBMF-223 also demonstrated a high bioavailaibity (>100%) in i.p. administration and low plasma protein binding (34%). Notably, the hTP inhibitor was able to reduce the relative tumor volume and the tumor growth rate, in both experimental models. In the glioblastoma model, the inhibition rate was 31% in male mice, and 50% in the colorectal model. For female, the percentage of reduction was 50% in the colorectal model. Interestingly, in both in vivo models, CPBMF-223 was able to decrease the tumors number of blood vesses and did not modify the liver injury enzymes. Collectively, the resuts bring new evidence of the toxicological safety of the CPBMF-223 compound and the antitumor activity performed in in vivo cancer models, pointing out this inhibitor as a promising drug to cancer treatment.
publishDate 2020
dc.date.accessioned.fl_str_mv 2020-10-26T19:53:44Z
dc.date.issued.fl_str_mv 2020-03-27
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dc.publisher.department.fl_str_mv Escola de Medicina
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