Caffeine Clinical Trial
Official title:
Neuroplastic Alterations of the Motor Cortex by Caffeine: Differences Between Caffeine and Non-caffeine Users and Influence of Vigilance During Stimulation
Caffeine is a psychostimulant drug. It acts as a competitive antagonist at adenosine
receptors, which modulate cortical excitability as well. In deep brain stimulation (DBS), the
production of adenosine following the release of adenosine triphosphate (ATP) explains the
reduction of tremor. Binding of adenosine to adenosine A1 receptors suppresses excitatory
transmission in the thalamus and hereby reduces both tremor-and DBS-induced side effects.
Also, the effect of adenosine was attenuated following the administration of the
8-Cyclopentyl-1,3-dipropylxanthine (DPCPX) adenosine A1 receptor antagonist. Therefore, the
presence of a receptor antagonist such as caffeine was suggested to reduce the effectiveness
of deep brain stimulation (DBS) in treating tremor and other movement disorders.
Based on this finding, the investigators hypothesize that the antagonistic effect of caffeine
can tentatively block the excitatory effects of transcranial alternating current stimulation
(tACS). The plasticity effects might differ among caffeine users and non- caffeine users
depending on the availability of receptor binding sites.
Apart from that, a major issue in NIBS studies including those studying motor-evoked
potentials is the response variability both within and between individuals. The trial to
trial variability of motor evoked potentials (MEPs) may be affected by many factors. Inherent
to caffeine is its effect on vigilance. In this study, the investigator shall monitor the
participant's vigilance by pupillometry to (1) better understand the factors, which might
cause variability in transcranial excitability induction studies and (2) to separate the
direct pharmacological effect from the indirect attentional effect of caffeine.
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