Chronic Treatment of C6 Glioma Cells with Antidepressant Drugs Results in a Redistribution of Gsα
2001
Previous studies have demonstrated that chronic treatment of C6 glioma cells with the antidepressants desipramine and fluoxetine increases the Triton X-100 solubility of the G protein Gsα (Toki et al., 1999). The antidepressants also caused a 50% decrease in the amount of Gsα localized to caveolae-enriched membrane domains. In this study, laser scanning confocal microscopy reveals that Gsα is localized to the plasma membrane as well as the cytosol in both treated and control cells. However, striking differences are seen in the distribution of Gsα in the long cellular processes after chronic treatment with these antidepressant drugs. Control cells display Gsα along the entire process with an especially high concentration of that G protein at the distal ends. Desipramine- or fluoxetine-treated cells show a more centralized clustering of Gsα in the Golgi region of the cell and a drastic reduction of Gsα in the cellular processes. There is no change in the distribution of Goα after desipramine treatment and the antipsychotic drug chlorpromazine does not alter Gsα. These results suggest that antidepressant-induced changes in the association of Gsα with the plasma membrane may translate into altered cellular localization of this signal transducing protein. Thus, modification of the coupling between Gs-coupled receptors and adenylyl cyclase may underlie both antidepressant therapy and depressive illnesses. This report also suggests that modification of the membrane domain occupied by Gsα might represent a mechanism for chronic antidepressant effects.
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