Mechanism of action for the cytotoxic effects of the nitric oxide prodrug JS-K in murine erythroleukemia cells

Article ID	Journal	Published Year	Pages	File Type
2136998	Leukemia Research	2014	6 Pages	PDF

Abstract

The nitric oxide (NO) prodrug JS-K, a promising anti-cancer agent, consists of a diazeniumdiolate group necessary for the release of NO as well as an arylating ring. In this study, we research the mechanism by which JS-K kills a murine erythroleukemia cell line and determine the roles of NO and arylation in the process. Our studies indicate that JS-K inhibits the PI 3-kinase/Akt and MAP kinase pathways. This correlates with the activation of the tumor suppressor FoxO3a and increased expression of various caspases, leading to apoptosis. The arylating capability of JS-K appears to be sufficient for inducing these biological effects. Overall, these data suggest that JS-K kills tumor cells by arylating and inactivating signaling molecules that block the activation of a tumor suppressor.

Keywords

FOXO3a JS-K Murine erythroleukemia cells Apoptosis

Related Topics

Life Sciences Biochemistry, Genetics and Molecular Biology Cancer Research

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Mechanism of action for the cytotoxic effects of the nitric oxide prodrug JS-K in murine erythroleukemia cells

Authors

Monika Z. Kaczmarek, Ryan J. Holland, Stephen A. Lavanier, Jami A. Troxler, Valentyna I. Fesenkova, Charlotte A. Hanson, Joan L. Cmarik, Joseph E. Saavedra, Larry K. Keefer, Sandra K. Ruscetti,