Dopamine Release and Uptake Dynamics within Nonhuman Primate Striatum<i>In Vitro</i>

Cragg, Stephanie J.; Hille, Christopher J.; Greenfield, Susan

doi:10.1523/jneurosci.20-21-08209.2000

Cited by 95 publications

(127 citation statements)

References 71 publications

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“…Although previous work had shown that dopamine release and uptake share many characteristics in the putamen and caudate, there seems to be a continuum of distinct functional domains from ventral to dorsal areas within these two brain regions, with dopamine release and uptake being significantly greater in the dorsal compared with the ventral regions (Cragg et al, 2000(Cragg et al, , 2002. We therefore investigated ␣3/␣6␤2* and ␣4␤2* nAChR-modulated functional properties in the ventral and dorsal striatal areas, with a focus on the putamen because it is more vulnerable in Parkinson's disease (Hornykiewicz, 2001).…”

Section: ␣3/␣6␤2* Nachr Blockade Results In a Major Decrease In Evokementioning

confidence: 83%

“…Moreover, this anatomical diversity is associated with heterogeneity in striatal dopamine function (Cragg et al, 2000;McCallum et al, 2006b). The heterogeneous nature of the putamen is further illustrated by findings that there is a clear ventral-to-dorsal gradient in striatal dopaminergic cell loss with denervation (Song and Haber, 2000;McCallum et al, 2006b).…”

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confidence: 99%

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Prominent Role of α3/α6β2^*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

et al. 2009

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Brain dopaminergic systems are critical in motor control as evidenced by findings that their disruption results in movement disorders such as Parkinson's disease. Nicotinic acetylcholine receptor (nAChR) activation plays an important role in regulating striatal dopaminergic function. Rodent studies show that short-term nicotine exposure influences stimulated striatal dopamine release with responsiveness dependent on neuronal activity. However, studies have not yet been done in nonhuman primates, nor has work been done to evaluate the effect of long-term nicotine exposure, which is relevant for therapies for chronic neurological disorders. Here, we used voltammetry to assess the role of nAChRs on evoked dopamine release from monkey putamen slices. In both ventral and dorsal putamen, ␣3/␣6␤2* nAChRs regulated Ն80% of non-burst-(single pulse) nAChR-modulated dopamine release, and ␣4␤2* nAChRs regulated the remainder. Similar results were observed with burstfiring in ventral but not dorsal putamen, indicating that nAChRmodulated effects on release depend on the subregion and firing frequency. Next, we investigated the consequence of long-term nicotine exposure via the drinking water on nAChR-modulated responsiveness. Nicotine treatment altered both non-burst-and burst-stimulated dopamine release in ventral but not dorsal putamen. Altogether, these data support a predominant role for ␣3/ ␣6␤2* nAChRs in the regulation of evoked dopamine release in nonhuman primate putamen. They also show that long-term nicotine treatment selectively modifies nAChR-modulated release in distinct striatal subregions. These findings have implications for the development of treatments for addiction and neurological disorders with nAChR dysfunction.The nigrostriatal dopaminergic system plays a critical role in motor function under physiological conditions and in neurodegenerative disorders such as Parkinson's disease. Striatal dopaminergic afferents are in intimate contact with numerous neuronal elements from other neurotransmitter systems, including those of the cholinergic system (Zhou et al., 2002;. Indeed, there exists an extensive overlap of dopaminergic and cholinergic markers in the striatum, providing the anatomical basis for the close functional interrelationship between these two neurotransmitter systems (Zhou et al., 2002).Acetylcholine, secreted from cholinergic interneurons, modulates striatal dopamine release primarily via activation of nicotinic acetylcholine receptors (nAChRs), which are pentameric ligand-gated ion channels. The principal nAChRs in the striatum are the ␣4␤2* and ␣6␤2* subtypes (the asterisk denotes the possible presence of other subunits in the receptor complex) Quik et al., 2007;. Receptor expression studies in rodents indicate that ␣4␤2* nAChRs are in the majority (ϳ85%) compared with the ␣6␤2* nAChR subtype (ϳ15%). However, functional studies (synaptosomal nAChR-evoked [ 3 H]dopamine release) show that ␣4␤2* nAChRs control only ϳ70% and ␣6␤2* nAChRs 30% of striatal dopamine release. This discrepa...

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Section: ␣3/␣6␤2* Nachr Blockade Results In a Major Decrease In Evokementioning

confidence: 83%

mentioning

confidence: 99%

Prominent Role of α3/α6β2^*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

et al. 2009

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“…[60][61][62] The dynamics of dopamine release, uptake kinetics, regulation by firing frequency and presynaptic autoreceptor function in the human striatum, which consists of a distinct caudate nucleus and putamen, also differs considerably from rodent striatum. 63,64 Hence, the pharmacological response in cortical or striatal sites to antipsychotic drugs may be different in primate brain than in mouse brain resulting in potentially different transcriptome profiles.…”

Section: Discussionmentioning

confidence: 99%

Antipsychotic drug treatment alters expression of mRNAs encoding lipid metabolism-related proteins

et al. 2003

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Using an automated PCR-based genomics approach, TOtal Gene expression Analysis (TOGA s ), we have examined gene expression profiles of mouse striatum and frontal cortex in response to clozapine and haloperidol drug treatment. Of 17 315 mRNAs observed, TOGA s identified several groups of related molecules that were regulated by drug treatment. The expression of some genes encoding proteins involved in neurotransmission, signal transduction, oxidative stress, cell adhesion, apoptosis and proteolysis were altered in the brains of both clozapine-and haloperidol-treated mice as recognized by TOGA s . Most notable was the differential expression of those genes whose products are associated with lipid metabolism. These include apolipoprotein D (apoD), the mouse homolog of oxysterol-binding protein-like protein 8 (OSBPL8), a diacylglycerol receptor (n-chimerin), and lysophosphatidic acid (LPA) acyltransferase. Real-time PCR analysis confirmed increases in the RNA expression of apoD (1.6-2.2-fold) and OSBPL8 (1.7-2.6-fold), and decreases in the RNA expression of nchimerin (1.5-2.2-fold) and LPA acyltransferase (1.5-fold) in response to haloperidol and/or clozapine treatment. Additional molecules related to calcium homeostasis and signal transduction, as well as four sequences of previously unidentified mRNAs, were also confirmed by real-time PCR to be regulated by drug treatment. While antipsychotic drugs may affect several metabolic pathways, lipid metabolism/signaling pathways may be of particular importance in the mechanisms of antipsychotic drug action and in the pathophysiology of psychiatric disorders. Molecular Psychiatry (2003) 8, 983-993.

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“…Although stimulation-evoked release has been measured from monkey striatum in vitro using voltammetry (Cragg et al, 2000) and, more recently, nicotine-stimulated release has been measured in vivo with positron emission tomography (Marenco et al, 2004), nicotine-evoked [ 3 H]dopamine release from synaptosomes has not previously been studied using monkey brain, although this approach is widely used with rodent preparations (Wonnacott, 1997;Grady et al, 2001;Champtiaux et al, 2003;Quik et al, 2003). Because this technique offers the advantage that it allows for the quantitative determination of evoked-release under well defined experimental conditions, we conducted experiments to establish its feasibility using monkey synaptosomes.…”

Section: Characterization Of Nicotine-evoked [ 3 H]dopamine Release Fmentioning

confidence: 99%

“…Stimulation-evoked release has previously been measured from control monkey striatum in vitro using voltammetry (Cragg et al, 2000); nicotine-stimulated release has been measured in vivo with positron emission tomography (Marenco et al, 2004). However, nicotine-evoked […”

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confidence: 99%

Decrease in α3^/α6^Nicotinic Receptors but Not Nicotine-Evoked Dopamine Release in Monkey Brain after Nigrostriatal Damage

et al. 2005

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Nicotinic acetylcholine receptors (nAChRs) are decreased in the striata of patients with Parkinson's disease (PD) or in experimental models after nigrostriatal damage. Because presynaptic nAChRs on striatal dopamine terminals mediate dopamine release, receptor loss may contribute to behavioral deficits in PD. The present experiments were done to determine whether nAChR function is affected by nigrostriatal damage in nonhuman primates, because this model shares many features with PD. Initial characterization of nicotine-evoked [ 3 H]dopamine release from monkey striatal synaptosomes revealed that release was calcium-dependent and inhibited by selective nAChR antagonists. It is noteworthy that a greater proportion (ϳ70%) of release was inhibited by the ␣3*/␣6* antagonist ␣-conotoxinMII (␣-CtxMII) compared with rodents. Monkeys were lesioned with 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP), and [ 3 H]dopamine release, dopamine transporter, and nAChRs were measured. As anticipated, lesioning decreased the transporter and ␣3*/␣6* nAChRs in caudate and putamen. In contrast, ␣3*/␣6* nAChR-evoked [ 3 H]dopamine release was reduced in caudate but not putamen, demonstrating a dissociation between nAChR sites and function. A different pattern was observed in the mesolimbic dopamine system. Dopamine transporter levels in nucleus accumbens were not reduced after MPTP, as expected; however, there was a 50% decline in ␣3*/␣6* nAChR sites with no decrease in ␣3*/␣6* receptor-evoked dopamine release. No declines in ␣-CtxMIIresistant nAChR (␣4*) binding or nicotine-evoked release were observed in any region. These results show a selective preservation of ␣3*/␣6* nAChR-mediated function in the nigrostriatal and mesolimbic dopamine systems after nigrostriatal damage. Maintenance of function in putamen, a region with a selective loss of dopaminergic terminals, may be important in PD.Parkinson's disease (PD) is characterized by motor and cognitive deficits and is manifested by reductions in dopaminergic neurons in substantia nigra and dopamine levels in striatum (Olanow, 2004). PD is also associated with decreases in striatal nicotinic acetylcholine receptors (nAChRs), including those containing ␣4*, ␣3*, and/or ␣6* but not ␣7* subunits (* denotes nicotinic receptors containing the indicated ␣ and/or ␤ subunit and also additional undefined subunits; Quik, 2004). Similar declines in nAChRs in Parkinsonian animal models support these findings (Quik et al., 2001(Quik et al., , 2003Champtiaux et al., 2002;Kulak et al., 2002;Zoli et al., 2002).Receptor binding and immunoprecipitation studies have revealed multiple nAChR subtypes on striatal dopaminergic terminals, including both ␣4* and ␣6* in rodents (Klink et al., 2001;Champtiaux et al., 2002Champtiaux et al., , 2003Zoli et al., 2002;Cui et al., 2003) and ␣3*, ␣4*, and ␣6* in monkeys Quik et al., 2001Quik et al., , 2002Quik et al., , 2005. In monkey, moderate nigrostriatal damage induced by the dopaminergic toxin 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) prefer...

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Dopamine Release and Uptake Dynamics within Nonhuman Primate StriatumIn Vitro

Cited by 95 publications

References 71 publications

Prominent Role of α3/α6β2^*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

Prominent Role of α3/α6β2^*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

Antipsychotic drug treatment alters expression of mRNAs encoding lipid metabolism-related proteins

Decrease in α3^/α6^Nicotinic Receptors but Not Nicotine-Evoked Dopamine Release in Monkey Brain after Nigrostriatal Damage

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Dopamine Release and Uptake Dynamics within Nonhuman Primate StriatumIn Vitro

Cited by 95 publications

References 71 publications

Prominent Role of α3/α6β2*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

Prominent Role of α3/α6β2*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

Antipsychotic drug treatment alters expression of mRNAs encoding lipid metabolism-related proteins

Decrease in α3*/α6*Nicotinic Receptors but Not Nicotine-Evoked Dopamine Release in Monkey Brain after Nigrostriatal Damage

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Prominent Role of α3/α6β2^*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

Prominent Role of α3/α6β2^*nAChRs in Regulating Evoked Dopamine Release in Primate Putamen: Effect of Long-Term Nicotine Treatment

Decrease in α3^/α6^Nicotinic Receptors but Not Nicotine-Evoked Dopamine Release in Monkey Brain after Nigrostriatal Damage