Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
6019514 | Experimental Neurology | 2008 | 10 Pages |
Abstract
Multiple targets and pathways may be amenable to the development of gene therapy approaches for Parkinson's disease. This article discusses some of the cellular and brain circuit pathways relevant to Parkinson's disease that would be clinically amenable to gene therapy. Approaches could be classified according to two main categories, i.e. symptomatic vs. neuroprotective/neurorestorative strategies. Examples of the different possibilities currently in development are given and feature both dopaminergic and non-dopaminergic symptomatic treatments of parkinsonian symptoms and/or l-DOPA-induced side effects, anti-apoptotic neuroprotective strategies and growth-factor delivery for neuroprotection/neurorestoration. While gene therapy has been mostly used so far for enhancing the expression of the target gene, the use of dominant negative or siRNA opens new possibilities. This, combined with the key feature of gene delivery that offers access to intracellular signalling pathways, is likely to further expand the number of proposed targets to be studied.
Keywords
GAD65HSVGad67MPTPAdVSTNAAVGPiIAPGDNFBH4tetrahydrobiopterinVMAT-2XIAPGCHguanosine triphosphate cyclohydrolase Iinternal segment of globus pallidusexternal segment of globus pallidusGAD6-OHDALIDAADC6-HydroxydopamineGPE1-methyl-4-phenyl-1,2,3,6-tetrahydropyridineglutamic acid decarboxylasel-3,4-dihydroxyphenylalaninel-DOPAAdenovirusaromatic l-amino acid decarboxylaseStriatumγ-aminobutyric acidDopamine transmissionParkinson's diseasesubstantia nigratyrosine hydroxylaseApoptosisCNSL-DOPA-induced dyskinesiacentral nervous systembasal gangliaGrowth factorGlial cell line-derived neurotrophic factorVesicular monoamine transporter-2Subthalamic nucleusAdeno-associated virusLentivirusherpes simplex virusGABAGlobus pallidusdopamine D2 receptor
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Authors
Grégory Porras, Erwan Bezard,