Activation of oxidative stress response by hydroxyl substituted chalcones and cyclic chalcone analogues in mitochondria.

We investigated the effect of hydroxyl substituted chalcone (1a) and some chalcone analogues (1b-d) on isolated rat liver mitochondria to gain new insights into the cytotoxic mechanism of these compounds. We observed an inhibitory effect on phosphorylation and the partial uncoupling of compounds 1a and 1d. Increased radical generation and possible covalent interaction of the compounds with cellular thiols resulted in glutathione (GSH) depletion and modulation of the investigated mitochondrial activities. Disruption of interconnected mechanisms as electron transport chain and energetic metabolism, ROS production and insufficiency of antioxidant defensive system could lead to induction of cell death.

Comparison of effects of some cyclic chalcone analogues on selected mitochondrial functions.

In earlier studies, cytotoxity of chalcones (1) and cyclic chalcone analogues E-2-arylidene-tetralones (2) and -benzosuberones (3) towards various murine and human tumour cells has been tested. Preliminary biochemical investigations showed the compounds to inhibit protein and DNA syntheses. It was also found that the compounds affect the cellular thiol status of the treated cells. In order to gain new insights into the cytotoxic mechanism of the compounds effects of some previously investigated 2 and 3 derivatives on isolated rat liver mitochondria was investigated. It was found that the most cytotoxic compounds 2c and 3b significantly decreased the GSH level of the mitochondria. Incubation of the investigated chalcones with reduced GSH under cell-free conditions indicated spontaneous conjugation (non-redox) reaction at pH 7.4 and pH 9.0. Investigation of antioxidant capacity of the compounds by monitoring time course of the Fenton-reaction initiated in vitro degradation of 2-deoxyribose showed the compounds to display hydroxyl radical scavenger activity. Investigation of respiratory control ratio of 2c and 3b showed the compounds to display an inhibitory effect on respiration, compound 2b, however, displayed rather an uncoupling effect. The experiments provide further details of cytotoxic effects of the synthetic chalcones displaying dual - cytotoxic and cytoprotective - effects.