Haruko Kusumoto scite author profile

Abstract. Selegiline is used an adjunct to L-DOPA therapy. We investigated extracellular striatal dopamine (DA) level in awake rats treated with L-DOPA and/ or selegiline using a microdialysis method. Rats given 10 mg / kg, i.p. per day selegiline for 7 days were administered with a single dose of 100 mg / kg, i.p. L-DOPA 0 (3 h), 1, 3, 7, 14, 21, or 28 days after the last selegiline treatment. Carbidopa was administered 0.5 h before L-DOPA administration. The significant increase in basal DA level before L-DOPA treatment persisted until 1 day after the last selegiline treatment, and the significant decrease in basal DOPAC level persisted for more than 28 days. Thus, selegiline affected DA catabolism for more than 28 days. Total monoamine oxidase (MAO) and MAO-B activities at day 0 decreased by 22% and 5.7%, respectively. The significant enhancement of L-DOPA-induced increase in DA level was observed until 3 days after the last selegiline treatment. Next, the effects of reducing L-DOPA dose by 25% were examined 3 h after the last selegiline treatment. A dose-dependent decrease in DA level was observed, indicating that DA level in selegiline-treated rats can be controlled by L-DOPA dose.

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In vivo effects of a monoamionergic activity enhancer

Ishibashi¹,

Tsunekawa²,

Kusumoto³

et al. 2007

Neuroscience Research

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Haruko Kusumoto

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In vivo effects of a monoamionergic activity enhancer

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