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Dynamics of tyrosine hydroxylase mediated regulation of dopamine synthesis
Authors:Poorvi Kaushik  Fredric Gorin  Shireen Vali
Affiliation:(1) Cellworks Group Inc., 13962 Pierce Road, Saratoga, CA 95070, USA;(2) Department of Neurology and the Center for Neuroscience, University of California Davis, Davis, CA 95616,, USA
Abstract:
Tyrosine hydroxylase's catalysis of tyrosine to dihydroxyphenylalanine (DOPA) is the highly regulated, rate-limiting step catalyzing the synthesis of the catecholamine neurotransmitter dopamine. Phosphorylation, cofactor-mediated regulation, and the cell's redox status, have been shown to regulate the enzyme's activity. This paper incorporates these regulatory mechanisms into an integrated dynamic model that is capable of demonstrating relative rates of dopamine synthesis under various physiological conditions. Most of the kinetic equations and substrate parameters used in the model correspond with published experimental data, while a few which were not available in literature have been optimized based on explicit assumptions. This kinetic pathway model permits a comparison of the relative regulatory contributions made by variations in substrate, phosphorylation, and redox status on enzymatic activity and permits predictions of potential disease states. For example, the model correctly predicts the recent observation that individuals with haemochromatosis and having excessive iron accumulation are at increased risk for acquiring Parkinsonism, a defect in neuronal dopamine synthesis (Bartzokis et al., 2004; Costello et al., 2004). Alpha synuclein mediated regulation of tyrosine hydroxylase has also been incorporated in the model, allowing an insight into the over-expression and aggregation of alpha synuclein in Parkinson's disease. Action Editor: Upinder Bhalla
Keywords:Tyrosine hydroxylase  Dopamine biosynthesis  Phosphorylation  Parkinson's disease  Iron  Alpha synuclein  Kinetic model
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