Parkinson's Disease Clinical Trial
Official title:
Caffeine for Motor Manifestations of Parkinson's Disease: An Open-Label Dose-Response Study.
Numerous epidemiological studies have linked lifelong use of caffeine to a lower risk of
Parkinson's disease (PD) - prospective studies have estimated that non-coffee drinkers have
an approximately 1.7-2.5 fold increased risk of developing PD compared to coffee drinkers.
This is an extremely important finding which deserves further more in depth investigations.
The exact pathophysiological mechanism remains elusive, but multiple hypotheses do exist:
Caffeine antagonizes adenosine receptors directly yielding an improvement on motor systems
and even on Levodopa serum concentrations (when on therapy). An additional explanation is
that adenosine antagonism has neuroprotective properties by acting locally on basal ganglia
circuits and the substantia nigra.
The current study aims to identify the optimal caffeine dose with maximal motor benefit and
the least amount of undesirable adverse effects.
Caffeine has been in widespread use for centuries, and is the commonest psychostimulant used
worldwide. In Canada, estimates of mean daily intake for a 70 kg person range from 200-450
mg. The main sources of caffeine ingestion are in beverages - depending on brewing technique
a typical cup of drip-filtered coffee can contain between 100 and 150 mg of caffeine
(gourmet drip coffees contain up to 300 mg and espresso preparations generally contain much
less caffeine). Black tea contains between 30 and 50 mg, and lower amounts of caffeine are
found in soft drinks, green teas, and chocolate. Caffeine is a substance with a well-defined
effect and side-effect profile, and in general it is very well tolerated. Side effects can
include irritability, insomnia, enhancement of physiologic tremor, and stomach upset. Abrupt
withdrawal from caffeine can cause headache and excessive sleepiness. Caffeine can
exacerbate pre-existing supraventricular tachycardia. Multiple large-scale epidemiologic
studies have not found evidence for adverse health effects with long-term moderate use of
caffeine. Caffeine has a T-max of approximately 1 hour and readily crosses the blood brain
barrier. It has first order kinetics. Plasma half life estimates range from 3-6 hours,
increased in the case of pregnancy or severe liver disease. Drug interactions are uncommon:
Caffeine withdrawal may cause lithium toxicity, and caffeine increases clozapine levels.
CNS effects of caffeine are mainly due to antagonism of the A1 and A2A adenosine receptors,
(A2A predominates in the striatum). Potential effects upon motor manifestations of PD are
predominantly related to the antagonistic action of adenosine on dopamine release in the
striatum. Partial tolerance to CNS effects is common, and begins to occur within one week
(tolerance is more pronounced for the A1 receptor, suggesting that motor changes may show
less tolerance). If effective for PD, caffeine has the potential to be a very important
advance for patient care, for numerous reasons. First of all, it has been in widespread use
for centuries, so the long-term safety has been determined. Caffeine is widely available as
tablets which are very inexpensive (i.e. less than 25 cents per tablet), potentially
resulting in substantial cost savings for patients and health-care planners. Caffeine also
has the potential (as yet unproven) to treat non-motor manifestations of PD, particularly
excessive daytime somnolence.
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Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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