Literature DB >> 23288971

Increased synaptic dopamine in the putamen in restless legs syndrome.

Christopher J Earley1, Hiroto Kuwabara, Dean F Wong, Charlene Gamaldo, Rachel E Salas, James R Brašić, Hayden T Ravert, Robert F Dannals, Richard P Allen.   

Abstract

STUDY
OBJECTIVES: Prior studies using positron emission tomography (PET) or single-photon emission computed tomography techniques have reported inconsistent findings regarding differences between patients with restless legs syndrome (RLS) and control patients in the striatal dopamine-2 receptor (D2R) binding potentials (BP). D2R-BP does reflect receptor-ligand interactions such as receptor affinity (K(d)) and density (β(max)) or neurotransmitter synaptic concentrations. Thus, differences in D2R-BP reflect changes in these primary factors. PET techniques are currently available to estimate D2R β(max) and K(d).
DESIGN: Separate morning and evening PET scans were performed. The D2R-BP were measured in basal ganglia using [(11)C]raclopride.
SETTING: Academic medical center. PATIENTS OR PARTICIPANTS: Thirty-one patients with primary RLS and 36 age- and sex-matched control patients completed the study. MEASURES AND
RESULTS: Patients with RLS had lower D2R-BP in putamen and caudate but not the ventral striatum. A subgroups analysis of those RLS patients who had not previously taken dopaminergic medications continued to show a significantly lower D2R-BP in the posterior putamen. D2R-BP did not differ between night and day for either group. D2R β(max) and K(d) did not differ significantly between patients with RLS and control patients but did show a strong and significant increase at night in the ventral striatum. Primary and secondary clinical measures of disease status failed to show any relation to D2R in any brain region.
CONCLUSIONS: Given the lack of any difference in either β(max) or K(d) and the prior studies supporting an increase in presynaptic dopaminergic activity, the current changes found in D2R-BP likely reflect an increase in synaptic dopamine.

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Year:  2013        PMID: 23288971      PMCID: PMC3524542          DOI: 10.5665/sleep.2300

Source DB:  PubMed          Journal:  Sleep        ISSN: 0161-8105            Impact factor:   5.849


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