Induction of dopamine biosynthesis by l-DOPA in PC12 cells: Implications of l-DOPA influx and cyclic AMP
2008
Abstract The effects of 3,4-dihydroxyphenylalanine ( l -DOPA) on dopamine biosynthesis and cytotoxicity were investigated in PC12 cells. l -DOPA treatment (20–200 μM) increased the levels of dopamine by 226%–504% after 3–6 h of treatment and enhanced the activities of tyrosine hydroxylase (TH) and aromatic l -amino acid decarboxylase (AADC). l -DOPA (20–200 μM) treatment led to a 562%–937% increase in l -DOPA influx at 1 h, which inhibited the activity of TH, but not AADC, during the same period. The extracellular releases of dopamine were also increased by 231%–570% after treatment with 20 and 200 μM l -DOPA for 0.5–3 h. l -DOPA at a concentration of 100–200 μM, but not 20 μM, exerted apoptotic cytotoxicity towards PC12 cells for 24–48 h. l -DOPA (20–200 μM) increased the intracellular cyclic AMP levels by 318%–557% after 0.5–1 h in a concentration-dependent manner. However, the elevated cyclic AMP levels by l -DOPA could not protect against l -DOPA (100–200 μM)-induced cytotoxicity after 24–48 h. In addition, l -DOPA (20–200 μM)-induced increases in cyclic AMP and dopamine were significantly reduced by treatment with SCH23390 (dopamine D 1 receptor antagonist). The increased levels of dopamine by l -DOPA were also reduced by H89 (protein kinase A, PKA, inhibitor) and GF109203X (protein kinase C inhibitor); however, the reduction by GF109203X was not significant. l -DOPA at 20–200 μM stimulated the phosphorylation of PKA and cyclic AMP-response element binding protein and induced the biosynthesis of the TH protein. These results indicate that 20–200 μM l -DOPA induces dopamine biosynthesis by two pathways. One pathway involves l -DOPA directly entering the cells to convert dopamine through AADC activity ( l -DOPA decarboxylation). The other pathway involves l -DOPA and/or released dopamine activating TH to enhance dopamine biosynthesis by the dopamine D 1 receptor-cyclic AMP–PKA signaling system (dopamine biosynthesis by TH).
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