Parkinson's Disease Clinical Trial
Official title:
Apomorphine Effect on Nociceptive Perception in Parkinson's: a Clinical and Imaging Study.
Patients suffering from Parkinson's disease (PD) frequently experienced painful sensations. We suppose that painful symptoms could be related to the neurotransmitter deficit of PD. So, we would like to evaluate the involvement of dopaminergic system in nociceptive processing in PD patients. The objectives of this study is to assess and to compare the effect of a dopamine agonist administration on the nociceptive threshold and on the cerebral activity using positrons emission tomography (PET scan) in two groups of PD patients (in 16 painful PD patients and in 16 pain free PD patients). We hypothesise that dopamine agonist could normalise nociceptive threshold and cerebral activity which were both abnormal in PD patients. Moreover, we think that painful PD patients could be more improved by dopamine agonist than pain free PD patients.
Patients suffering from Parkinson's disease (PD) frequently experienced painful sensations.
Painful complaints with various description (muscle cramps, painful dystonia, aching,
numbness, tingling, burning, vibrating, lancinating) are described and can or cannot be
related to motor symptoms. Physiopathology of pain in PD is discussed. It has been suggested
that the occurrence of painful symptoms could be in part due to central modification of
nociception and basal ganglia damage and the dopaminergic deficit would be expected to
eliminate the inhibitory influence on thalamic nociceptive activity. Recently, data have
shown that PD patient had a lower nociceptive threshold than healthy volunteers. Our team
has reported that levodopa administration normalised this nociceptive threshold and
decreased cerebral activity measured with positrons emission tomography (PET- H215O during
experimental nociceptive stimulation) in several nociceptive cortical areas which were
overactive in PD. These findings suggest that central dopamine system plays an important
part in the control of the nociceptive pathways in PD. Nevertheless, in the central nervous
system, levodopa could be converted in dopamine but also in noradrenaline modulating
noradrenergic system. In order to confirm the involvement of dopaminergic system in
nociceptive processing in PD, we would like to assess a specific drug of dopamine system (a
dopamine agonist, apomorphine) in PD patients.
The primary objective of this study is to assess the effect of dopamine agonist acute
administration versus placebo on the nociceptive subjective threshold in two groups of PD
patients (painful PD patients, n =16 and pain free PD patients, n = 16). This is a
controlled cross over, double blind, randomised study.
The secondary objectives are to assess and to compare the apomorphine effect on the
objective nociceptive threshold (nociceptive flexion reflex) and on the activation of
cerebral areas using functional imaging (TEP- H215O) during experimental nociceptive
stimulation in the two groups of PD patients.
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Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Basic Science
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