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. 2006 Oct;14(4):564-70.
doi: 10.1016/j.ymthe.2006.05.005. Epub 2006 Jul 7.

Long-term clinical improvement in MPTP-lesioned primates after gene therapy with AAV-hAADC

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Free article

Long-term clinical improvement in MPTP-lesioned primates after gene therapy with AAV-hAADC

Krystof S Bankiewicz et al. Mol Ther. 2006 Oct.
Free article

Abstract

Dopamine, the major neurotransmitter depleted in Parkinson disease, can be synthesized and regulated in vivo with a combination of intrastriatal AAV-hAADC gene therapy and administration of the dopamine precursor l-Dopa. When tested in MPTP-lesioned monkeys, this approach resulted in long-term improvement in clinical rating scores, significantly lowered l-Dopa requirements, and a reduction in l-Dopa-induced side effects. Positron emission tomography with [(18)F]FMT confirmed persistent AADC activity, demonstrating for the first time that infusion of AAV vector into primate brain results in at least 6 years of transgene expression. AAV-hAADC restores the ability of the striatum to convert l-Dopa into dopamine efficiently. Introduction of this therapy into the clinic holds promise for Parkinson patients experiencing the motor complications that result from escalating l-Dopa requirements against a background of disease progression.

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