Antineoplastic activity of the thiazolo[5,4-b]quinoline derivative D3CLP in K-562 cells is mediated through effector caspases activation

Por: Gonzalez-Sanchez, I, Solano, JD, Loza-Mejia, MA, Olvera-Vazquez, S, Rodriguez-Sotres, R, Moran, J, Lira-Rocha, A, Cerbon, MA

Publicada: 1 jun 2011

Web: https://www.scopus.com/inward/record.uri?eid=2-s2.0-79955608057&doi=10.1016%2fj.ejmech.2011.02.063&partnerID=40&md5=96f2b18d6e76102d44c4fcad19b12b3a

Resumen:
Thiazolo[5,4-b]quinolines are compounds structurally related to m-Amsacrine (m-Amsa), a potent antileukemic drug that intercalates to DNA and inhibits topoisomerase II in vitro inducing cell death. The clinical use of m-Amsa and other neoplastic drugs is limited due to side effects and drug resistance. In the present study we evaluated one thiazolo[5,4-b]quinoline derivate, 9-[(3-chloro)phenylamine]-2-[3-(diethylamine)propylamine]thiazolo[5,4-b] quinoline (D3CLP), considered isosteric with 9-anilinoacridines, in order to determine its relative cytotoxic activity in tumoral versus non-tumoral cells, as well as the cell death mechanism induced by D3CLP on K-562 human leukemia cells. D3CLP was found to be four times more cytotoxic to tumor cells than Peripheral Blood Monocyte Cells (PBMCs). On the other hand, D3CLP induces cell death without previous cell cycle arrest at any phase, as shown by flow cytometry after 12 h of exposure to this compound. Interestingly, we detected a subdiploid peak 24 h after treatment. Signs of apoptosis were evident, as detected by TUNEL positive cells, chromatin condensation and nuclear fragmentation. Effector caspases activation were assessed with peak activity at 24 h after treatment (as detected by fluorometry assays), at which time a subdiploid peak was found in flow cytometry histograms. All data are consistent with the induction of apoptotic cell death in K-562 cells via effector caspases activation. In conclusion, the significant cytotoxicity of D3CLP together with the cell death type it produces, justifies further experimental and preclinical evaluation of this compound in the effort to find new and highly specific anti-tumor agents against leukemia cells. © 2011 Elsevier Masson SAS.

Filiaciones:
Gonzalez-Sanchez, I:
Univ Nacl Autonoma Mexico, Dept Biol, Fac Quim, Mexico City 04510, DF, Mexico

Solano, JD:
Univ Nacl Autonoma Mexico, Dept Biol, Fac Quim, Mexico City 04510, DF, Mexico

Loza-Mejia, MA:
Univ Nacl Autonoma Mexico, Dept Farm, Fac Quim, Mexico City 04510, DF, Mexico

Olvera-Vazquez, S:
Univ Nacl Autonoma Mexico, Dept Farm, Fac Quim, Mexico City 04510, DF, Mexico

Rodriguez-Sotres, R:
Univ Nacl Autonoma Mexico, Dept Bioquim, Fac Quim, Mexico City 04510, DF, Mexico

Moran, J:
Univ Nacl Autonoma Mexico, Inst Fisiol Celular, Div Neurociencias, Mexico City 04510, DF, Mexico

Lira-Rocha, A:
Univ Nacl Autonoma Mexico, Dept Farm, Fac Quim, Mexico City 04510, DF, Mexico

Cerbon, MA:
Univ Nacl Autonoma Mexico, Dept Biol, Fac Quim, Mexico City 04510, DF, Mexico

ISSN: 02235234

EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY

Editorial
Elsevier Masson SAS, 23 RUE LINOIS, 75724 PARIS, FRANCE, Francia

Tipo de documento: Article
Volumen: 46 Número: 6
Páginas: 2102-2108

DOI: 10.1016/j.ejmech.2011.02.063

WOS Id: 000291118600018

ID de PubMed: 21420205

Antineoplastic activity of the thiazolo[5,4-b]quinoline derivative D3CLP in K-562 cells is mediated through effector caspases activation

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