Anti-liver cancer activity in vitro and in vivo induced by 2-pyridyl 2,3-thiazole derivatives

Silva, Thiago David dos Santos; Bomfim, Larissa Mendes; Rodrigues, Ana Carolina Borges da Cruz; Dias, Rosane Borges; Sales, Caroline Brandi Schlaepfer; Rocha, Clarissa Araújo Gurgel; Soares, Milena Botelho Pereira; Bezerra, Daniel Pereira; Cardoso, Marcos Veríssimo de Oliveira; Leite, Ana Cristina Lima; Militão, Gardenia Carmen Gadelha

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dc.contributor.author

Silva, Thiago David dos Santos

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Bomfim, Larissa Mendes

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Rodrigues, Ana Carolina Borges da Cruz

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Dias, Rosane Borges

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Sales, Caroline Brandi Schlaepfer

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Rocha, Clarissa Araújo Gurgel

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Soares, Milena Botelho Pereira

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Bezerra, Daniel Pereira

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Cardoso, Marcos Veríssimo de Oliveira

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Leite, Ana Cristina Lima

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Militão, Gardenia Carmen Gadelha

dc.creator

Silva, Thiago David dos Santos

dc.creator

Bomfim, Larissa Mendes

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Rodrigues, Ana Carolina Borges da Cruz

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Dias, Rosane Borges

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Sales, Caroline Brandi Schlaepfer

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Rocha, Clarissa Araújo Gurgel

dc.creator

Soares, Milena Botelho Pereira

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Bezerra, Daniel Pereira

dc.creator

Cardoso, Marcos Veríssimo de Oliveira

dc.creator

Leite, Ana Cristina Lima

dc.creator

Militão, Gardenia Carmen Gadelha

dc.date.accessioned

2018-05-04T14:23:31Z

dc.date.available

2018-05-04T14:23:31Z

dc.date.issued

2018-05-04

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(0041-008X) Toxicology and Applied Pharmacology

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http://repositorio.ufba.br/ri/handle/ri/25931

dc.description.abstract

A total of 24 hybrid compounds containing pyridyl and 1,3-thiazole moieties were screened against HL-60 (leukemia), MCF-7 (breast adenocarcinoma),HepG2 (hepatocellular carcinoma), NCI-H292 (lung carcinoma) human tumor cell lines and non-tumor cells (PBMC, human peripheral blood mononuclear cells). Most of them were highly potent in at least one cell line tested (IC50 ≤ 3 μM), being HL-60 the most sensitive and HepG2 the most resistant cell line. Among them, TAP-07 and TP-07 presented cytotoxic activity in all tumor cell lines, including HepG2 (IC50 2.2 and 5.6 μM, respectively) without antiproliferative effects to normal cells (PBMC) (IC50 N 30 μM),making TAP-07 and TP-07, the compounds with the most favorable selectivity index. TAP-07 and TP-07 induced apoptosis in HepG2 cells and presented in vivo antitumor activity in hepatocellular xenograft cancer model in C.B-17 severe combined immunodeficientmice. Systemic toxicological verified by biochemical and histopathological techniques reveled nomajor signs of toxicity after treatmentwith TAP-07 and TP-07. Together the results indicated the anti-liver cancer activity of 2-pyridyl 2,3-thiazole derivatives.

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Acesso Aberto

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dc.source

10.1016/j.taap.2017.06.003

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dc.subject

2-Pyridyl 2,3-thiazoles

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HepG2

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Cytotoxicity

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Antitumor

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Liver Cancer

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Toxicity

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dc.title

Anti-liver cancer activity in vitro and in vivo induced by 2-pyridyl 2,3-thiazole derivatives

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dc.type

Artigo de Periódico

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dc.identifier.number

329

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dc.publisher.country

Brasil

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ANTI-LIVER CANCER ACTIVITY IN VITRO AND IN VIVO INDUCED BY 2-PYRIDYL 2,3-THIAZOLE DERIVATIVES.pdf

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