Evaluation of Levodopa Dose and Magnitude of Dopamine Depletion as Risk Factors for Levodopa-Induced Dyskinesia in a Rat Model of Parkinson's Disease

Putterman, Daniel; Munhall, Adam C.; Kozell, Laura B.; Belknap, John K.; Johnson, Steven W.

doi:10.1124/jpet.107.126219

Cited by 72 publications

(58 citation statements)

References 41 publications

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“…S5C), consistent with the literature using this model (2,(30)(31)(32)(33)(34). Acute treatment with L-DOPA-induced pERK in predominantly medium-sized neurons and repeated L-DOPA administration reduced the number of medium-sized pERK-labeled cells by 72% and increased the number of large-diameter pERK-labeled neurons by 3.4-fold in lesioned striatum (Fig.…”

Section: Cholinergic Neuronal Hyperactivity Correlates With Lid In Unsupporting

confidence: 80%

“…Unilateral 6-OHDA lesions used in this study produced massive striatal DA depletions of 94%, covering the entire striatum, whereas striatal DA depletion is limited to the most dorsal aspect of dorsal striatum in Pitx3 ak/ak mice. LID has been reported with the first exposure to L-DOPA in unilateral 6-OHDA-lesioned rats (2,(30)(31)(32)(33)(34) and the level of dyskinetic behavior is influenced by the amount of DA loss (34). Therefore, we believe the Pitx3 ak/ak mice show the time course more consistent with mild to moderate PD, whereas 6-OHDAlesioned mice model a more severe stage of PD.…”

Section: Discussionmentioning

confidence: 72%

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Enhanced striatal cholinergic neuronal activity mediatesl-DOPA–induced dyskinesia in parkinsonian mice

Ding¹,

Won²,

Britt

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

170

192

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Treatment of Parkinson disease (PD) with L-3,4-dihydroxyphenylalanine (L-DOPA) dramatically relieves associated motor deficits, but L-DOPA-induced dyskinesias (LID) limit the therapeutic benefit over time. Previous investigations have noted changes in striatal medium spiny neurons, including abnormal activation of extracellular signal-regulated kinase1/2 (ERK). Using two PD models, the traditional 6-hydroxydopamine toxic lesion and a genetic model with nigrostriatal dopaminergic deficits, we found that acute dopamine challenge induces ERK activation in medium spiny neurons in denervated striatum. After repeated L-DOPA treatment, however, ERK activation diminishes in medium spiny neurons and increases in striatal cholinergic interneurons. ERK activation leads to enhanced basal firing rate and stronger excitatory responses to dopamine in striatal cholinergic neurons. Pharmacological blockers of ERK activation inhibit L-DOPA-induced changes in ERK phosphorylation, neuronal excitability, and the behavioral manifestation of LID. In addition, a muscarinic receptor antagonist reduces LID. These data indicate that increased dopamine sensitivity of striatal cholinergic neurons contributes to the expression of LID, which suggests novel therapeutic targets for LID.antagonist D opaminergic drugs are effective treatments for the motor symptoms of Parkinson disease (PD), but long-term therapy is limited by disabling abnormal involuntary movements, referred to as L-DOPA-induced dyskinesias (LID) (1). Thus, understanding the molecular and cellular mechanisms underlying LID will help identify more effective treatments for PD, and may also help elucidate the role of dopamine (DA) signaling in motor control.Several biochemical markers of LID have been studied in striatum using animal models. FosB/δFosB expression show a long-term temporal correlation with LID development in DA denervation PD models (2). The increased FosB expression persists over days or weeks and may contribute to the development of LID, but does not correlate with the L-DOPA-induced episodes of dyskinesia that follow each dose. To mediate expression of LID directly, cell signals should grow stronger with repeated L-DOPA treatment and show temporal correlation with acute dopaminergic stimulation. Acute administration of L-DOPA or dopamine agonists activates ERK1/2 by phosphorylation in striatal neurons of DA-denervated animals (3-7). In animals with unilateral 6-hydroxydopamine (6-OHDA) lesions, coadministration of inhibitors of ERK1/2 phosphorylation during repeated L-DOPA treatments reduce LID development (4,8). Studies on these molecular changes have focused on the predominant cell type in the striatum, medium spiny neurons (MSN). In addition, although the unilateral 6-OHDA lesion has been the standard model for the PD phenotype, and particularly for LID, the abrupt nature of the lesion and extreme depletion of dopaminergic afferents has posed limitations in behavioral and biochemical studies.In this study, we used both a unilateral 6-OHDA lesion model and a g...

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Section: Cholinergic Neuronal Hyperactivity Correlates With Lid In Unsupporting

confidence: 80%

Section: Discussionmentioning

confidence: 72%

Enhanced striatal cholinergic neuronal activity mediatesl-DOPA–induced dyskinesia in parkinsonian mice

Ding¹,

Won²,

Britt

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

170

192

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“…The fact that dyskinesia can emerge very quickly in severely affected or young people with PD is consistent with this argument, 10,11 as is the observation that dyskinesia can be seen with the first dose of levodopa in rodents and monkeys with toxin-induced parkinsonism. 12,13 The second important observation of this study is that the antiparkinsonian responses and the dyskinesia response evolved in a similar manner during the first 4 years of levodopa therapy. With time, both the increase in tapping speed and dyskinesia began with a shorter latency during the 2-hour levodopa infusions.…”

Section: Dyskinesia and Antiparkinsonian Responsementioning

confidence: 88%

Dyskinesia and the antiparkinsonian response always temporally coincide

Nutt

Chung²,

Holford

2010

Neurology

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Objective: To clinically characterize the temporal relationship between dyskinesia and the antiparkinsonian response when dyskinesia first emerges during long-term levodopa therapy and to determine if it is consistent with the hypothesized mechanism by which dyskinesia develops.Methods: Dyskinesia and the antiparkinsonian response to levodopa during 2-hour levodopa infusions were monitored at intervals through the first 4 years of long-term levodopa therapy in 20 subjects with idiopathic Parkinson disease (PD) and previously untreated with levodopa. The onset and offset of the antiparkinsonian response and dyskinesia were compared when dyskinesia first appeared during the 4 years. The findings were compared to 20 subjects with PD on longterm levodopa with dyskinesia and motor fluctuations. Results:The onset and offset of the antiparkinsonian response and dyskinesia generally coincided when dyskinesia first appeared during the 4 years and did not suggest any temporal dissociation of the 2 responses. Further, the latency to the onsets of dyskinesia and the antiparkinsonian response tended to shorten during long-term levodopa therapy, suggesting that both responses were sensitized by long-term levodopa. Conclusions:The similar onsets and offsets of the antiparkinsonian response and dyskinesia when dyskinesia first appears are not consistent with the postulated progressive decrease in threshold for dyskinesia during long-term levodopa therapy. Other mechanisms for the development of dyskinesia need to be considered. Neurology Levodopa-induced dyskinesia is postulated to result from repeated pulsatile dopaminergic stimulation which progressively lowers the threshold for dyskinesia by sensitization.1 At the beginning of levodopa therapy, the threshold for dyskinesia is much higher than the peak plasma levodopa concentrations. Conversely, the threshold for the antiparkinsonian response is envisioned to be lower than that for dyskinesia. The hypothesized different thresholds allow dissociation of the antiparkinsonian response and dyskinesia. Continued levodopa therapy lowers the threshold for dyskinesia and dyskinesia occurs briefly at peak concentrations. Eventually, similar concentrations produce dyskinesia and the antiparkinsonian response, making the responses inseparable ( figure 1A). This hypothesis assumes 1) the antiparkinsonian response and dyskinesia have distinctly different dose responses and 2) they are altered differently during long-term levodopa therapy.Evidence for this hypothesized scenario is from temporal extremes. Initial levodopa therapy rarely produces dyskinesia, consistent with a high threshold for dyskinesia.2,3 After years of levodopa therapy, dyskinesia and the antiparkinsonian response occur together, 2,3 e-Pub ahead of print on March 10, 2010, at www.neurology.org.

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“…Significant modifications from Cenci et al [9] include the use of males, altered lesion coordinates, desipramine to protect noradrenergic neurons, and a higher 6-OHDA dose. Our collaborators recently demonstrated that severe dopamine depletion is necessary but not sufficient to evoke dyskinesias and reviewed factors that may affect dyskinesia emergence [10].…”

Section: Discussionmentioning

confidence: 99%

Sigma ligands, but not N-methyl-D-aspartate antagonists, reduce levodopa-induced dyskinesias

Paquette¹,

Brudney

Putterman³

et al. 2008

NeuroReport

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Levodopa (L-DOPA) is the 'gold standard' to treat Parkinson's disease. Unfortunately, dyskinesias detract from its efficacy. Current dyskinesia treatments, including amantadine and dextromethorphan, are thought to work via N-methyl-D-aspartate (NMDA) antagonism, but this hypothesis has not been tested. The NMDA antagonists MK-801and HA-966 failed to suppress expression of dyskinesias in the 6-hydroxydopamine rat. Dyskinesias, however, were suppressed by the NMDA and sigma (σ)-1receptor ligand dextromethorphan and by the σ-1 antagonist BMY-14802. Antidyskinetic effects of dextromethorphan may be mediated via mechanisms other than NMDA, including the σ-1 receptor and other binding sites common to dextromethorphan and BMY-14802.

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Evaluation of Levodopa Dose and Magnitude of Dopamine Depletion as Risk Factors for Levodopa-Induced Dyskinesia in a Rat Model of Parkinson's Disease

Cited by 72 publications

References 41 publications

Enhanced striatal cholinergic neuronal activity mediatesl-DOPA–induced dyskinesia in parkinsonian mice

Enhanced striatal cholinergic neuronal activity mediatesl-DOPA–induced dyskinesia in parkinsonian mice

Dyskinesia and the antiparkinsonian response always temporally coincide

Sigma ligands, but not N-methyl-D-aspartate antagonists, reduce levodopa-induced dyskinesias

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