| Literature DB >> 26454648 |
Jamerson Ferreira de Oliveira1, Anekécia Lauro da Silva1, Débora Barbosa Vendramini-Costa2, Cezar Augusto da Cruz Amorim1, Júlia Furtado Campos3, Amélia Galdino Ribeiro1, Ricardo Olímpio de Moura4, Jorge Luiz Neves5, Ana Lúcia Tasca Gois Ruiz2, João Ernesto de Carvalho2, Maria do Carmo Alves de Lima6.
Abstract
A series of thiophene-2-thiosemicarbazones derivatives (5-14) was synthesized, characterized and evaluated for their antitumor activity. They were tested in vitro against human tumor cell lines through the colorimetric method. The results revealed that compounds 7 and 9 were the most effective in inhibiting 50% of the cell growth after 48 h of treatment. As compound 7 showed a potent antiproliferative profile, it has been chosen for further studies in 786-0 cell line by flow cytometry. Treatments with compound 7 (50 μM) induced early phosphatidylserine exposure after 18 h of exposure and this process progressed phosphatidylserine exposure with loss of cell membrane integrity after 24 h of treatment, suggesting a time-dependent cell death process. Regarding the cell cycle profile, no changes were observed after treatment with compound 7 (25 μM), suggesting a mechanism of cell death independent on the cell cycle. The in vivo studies show that compound 7 possess low acute toxicity, being the doses of 30-300 mgKg(-1) chosen for studies in Ehrlich solid tumor model in mice. All doses were able to inhibit tumor development being the lowest one the most effective. Our findings highlight thiophene-2-thiosemicarbazones as a promising class of compounds for further studies concerning new anticancer therapies.Entities:
Keywords: Antitumor; Cytotoxicity; Medicinal chemistry; Thiophene; Thiosemicarbazone
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Year: 2015 PMID: 26454648 DOI: 10.1016/j.ejmech.2015.09.036
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514