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Region-Specific Targets of p42/p44MAPK Signaling in Rat Brain
Authors:Ratan V. Bhat  Thomas M. Engber  James P. Finn  Elizabeth J. Koury  Patricia C. Contreras  Matthew S. Miller  Craig A. Dionne   Kevin M. Walton
Affiliation:Departments of Pharmacology and Cell Biology, Cephalon, West Chester, Pennsylvania, U.S.A.
Abstract:Abstract: In vitro studies indicate that p42/p44MAPK phosphorylate both nuclear and cytoplasmic proteins. However, the functional targets of p42/p44MAPK activation in vivo remain unclear. To address this question, we localized activated p42/p44MAPK in hippocampus and cortex and determined their signaling effects after electroconvulsive shock treatment (ECT) in rats. Phosphorylated p42/p44MAPK content increased in the cytoplasm of hippocampal neurons in response to ECT. Consistent with this cytoplasmic localization, inhibition of ECT-induced p42/p44MAPK activation by the extracellular signal-regulated kinase kinase inhibitor PD098059 blocked phosphorylation of the cytoplasmic protein microtubule-associated protein 2c (MAP2c), but failed to inhibit the induction of the nuclear protein c-Fos in response to ECT. In contrast to hippocampal neurons, cortical neurons exhibited an increase in amount of phosphorylated p42/p44MAPK in both the nucleus and cytoplasm after ECT. Accordingly, PD098059 blocked the induction of Fos-like immunoreactivity in the nuclei of cortical neurons as well as MAP2c phosphorylation in the cytoplasm. Our data indicate that both nuclear and cytoplasmic substrates can be activated by p42/p44MAPK in vivo. However, the functional targets of p42/p44MAPK signaling depend on the precise location of p42/p44MAPK within different subcellular compartments of brain regions. These results indicate unique functional pathways of p42/p44MAPK-mediated signal transduction within different brain regions in vivo.
Keywords:Signal transduction    Erk2    Mitogen-activated protein kinase    Hippocampus    Microtubule-associated protein 2    c-Fos    Phosphorylation    Neuronal function    Elk1    Cyclic AMP response element binding protein
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