Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia
L-dopa remains the most effective drug for improving motor symptoms of Parkinson's disease (PD). However, following long-term chronic treatment, the therapeutic effects of L-dopa are often accompanied by debilitating peak-dose dyskinesia. The mechanisms underlying L-dopa induced dyskinesia r...
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ndltd-UBC-oai-circle.library.ubc.ca-2429-164932018-01-05T17:38:25Z Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia Cheng, Christina L-dopa remains the most effective drug for improving motor symptoms of Parkinson's disease (PD). However, following long-term chronic treatment, the therapeutic effects of L-dopa are often accompanied by debilitating peak-dose dyskinesia. The mechanisms underlying L-dopa induced dyskinesia remain unknown. Rapid increases of dopamine (DA) in the severely DA denervated striatum are associated with L-dopa induced dyskinesia (Miller and Abercrombie, 1999). This DA efflux is believed to cause many post-synaptic changes that are associated with L-dopa induced dyskinesia (Olanow et al., 2000). Therefore, it is of interest to examine the underlying mechanisms of the L-dopa induced DA release. The objectives of the present experiments were to examine the role for the DA transporter (DAT) in mediating L-dopa-induced DA release. Firstly, systemic injection of a DAT antagonist, methylphenidate (MP) was used to assess the role of the DAT in L-dopa induced dyskinesia in chronically L-dopa treated animals. Results showed a dose-dependent effect of MP in the attenuation of L-dopa induced dyskinesia. Secondly, we investigated the functional mode of the DAT by examining the effects of MP pre-treatment on the L-dopa induced DA efflux and dyskinetic responses in three groups of rats 1) L-dopa-naive, 2) 1-week L-dopa treated, and 3) 3-week L-dopa treated, rats. MP pretreatment had no effect on L-dopa induced DA efflux in L-dopa naive, or 1 -week L-dopa treated animals. In contrast, systemic pretreatment of MP significantly attenuated the L-dopa induced DA response in 3-week treated rats, which was correlated with a similar decrease in L-dopa induced dyskinesia. The results from these experiments lend support to our hypothesis that reversal of the DAT through chronic L-dopa treatment contributes to the pathogenesis of L-dopa induced dyskinesia. Therefore, these findings suggest that the DAT is an important pharmacological target in the study and treatment of L-dopa induced dyskinesia. Medicine, Faculty of Graduate 2009-12-11T18:16:11Z 2009-12-11T18:16:11Z 2005 2005-11 Text Thesis/Dissertation http://hdl.handle.net/2429/16493 eng For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use. |
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NDLTD |
language |
English |
sources |
NDLTD |
description |
L-dopa remains the most effective drug for improving motor symptoms of Parkinson's
disease (PD). However, following long-term chronic treatment, the therapeutic effects of L-dopa
are often accompanied by debilitating peak-dose dyskinesia.
The mechanisms underlying L-dopa induced dyskinesia remain unknown. Rapid
increases of dopamine (DA) in the severely DA denervated striatum are associated with L-dopa
induced dyskinesia (Miller and Abercrombie, 1999). This DA efflux is believed to cause many
post-synaptic changes that are associated with L-dopa induced dyskinesia (Olanow et al., 2000).
Therefore, it is of interest to examine the underlying mechanisms of the L-dopa induced DA
release.
The objectives of the present experiments were to examine the role for the DA
transporter (DAT) in mediating L-dopa-induced DA release. Firstly, systemic injection of a
DAT antagonist, methylphenidate (MP) was used to assess the role of the DAT in L-dopa
induced dyskinesia in chronically L-dopa treated animals. Results showed a dose-dependent
effect of MP in the attenuation of L-dopa induced dyskinesia. Secondly, we investigated the
functional mode of the DAT by examining the effects of MP pre-treatment on the L-dopa
induced DA efflux and dyskinetic responses in three groups of rats 1) L-dopa-naive, 2) 1-week
L-dopa treated, and 3) 3-week L-dopa treated, rats. MP pretreatment had no effect on L-dopa
induced DA efflux in L-dopa naive, or 1 -week L-dopa treated animals. In contrast, systemic pretreatment
of MP significantly attenuated the L-dopa induced DA response in 3-week treated rats,
which was correlated with a similar decrease in L-dopa induced dyskinesia.
The results from these experiments lend support to our hypothesis that reversal of the
DAT through chronic L-dopa treatment contributes to the pathogenesis of L-dopa induced dyskinesia. Therefore, these findings suggest that the DAT is an important pharmacological
target in the study and treatment of L-dopa induced dyskinesia. === Medicine, Faculty of === Graduate |
author |
Cheng, Christina |
spellingShingle |
Cheng, Christina Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia |
author_facet |
Cheng, Christina |
author_sort |
Cheng, Christina |
title |
Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia |
title_short |
Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia |
title_full |
Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia |
title_fullStr |
Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia |
title_full_unstemmed |
Dopamine trasporter reversal as a pathogenic mechanism for L-dopa induced dyskinesia |
title_sort |
dopamine trasporter reversal as a pathogenic mechanism for l-dopa induced dyskinesia |
publishDate |
2009 |
url |
http://hdl.handle.net/2429/16493 |
work_keys_str_mv |
AT chengchristina dopaminetrasporterreversalasapathogenicmechanismforldopainduceddyskinesia |
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1718590237113843712 |