AI Article Synopsis

  • L-dopa is the most effective treatment for Parkinson's disease, but its long-term use can lead to dyskinesia, possibly due to heightened sensitivity of D1 dopamine receptors.
  • Research shows that while D1 receptor amounts stay the same in Parkinson’s, levels of downstream effectors like Galphaolf and Ggamma7 increase in patients' brains, influencing D1 receptor response.
  • This prolonged increase in Galphaolf levels may lead to persistent hypersensitivity of D1 receptors, contributing to complications from long-term L-dopa treatment.

Article Abstract

Although L-dopa remains the most effective treatment of Parkinson disease, its long-term administration is hampered by the appearance of dyskinesia. Hypersensitivity of dopamine D1 receptors in the striatum has been suggested to contribute to the genesis of these delayed adverse effects. However, D1 receptor amounts are unchanged in Parkinson disease, suggesting alterations of downstream effectors. In rodents, striatal D1 receptors activate adenylyl cyclase through olfactory type G-protein alpha subunit (Galphaolf) and G-protein gamma 7 subunit (Ggamma7). We found that Galphaolf was enriched in human basal ganglia and was markedly diminished in the putamen of patients with Huntington disease, in relation with the degeneration of medium spiny neurons. In contrast, in the putamen of patients with Parkinson disease, Galphaolf and Ggamma7 levels were both significantly increased. In the rat, the degeneration of dopamine neurons augmented Galphaolf levels in the striatal neurons, specifically at the plasma membrane, an effect accounting for the increase of D1 response on cAMP production in dopamine-depleted striatum. In lesioned rats, Galphaolf levels were normalized by a 3 week treatment with l-dopa or a D1 agonist but not with aD2-D3 agonist, supporting a Galphaolf regulation by D1 receptor usage. In contrast, the increases of Galphaolf levels in patients were not affected by the duration of l-dopa treatment but correlated with duration of disease. In conclusion, our results revealed in the parkinsonian putamen a prolonged elevation of Galphaolf levels that may lead to a persistent D1 receptor hypersensitivity and contribute to the genesis of long-term complications of L-dopa.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6729591PMC
http://dx.doi.org/10.1523/JNEUROSCI.0676-04.2004DOI Listing

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