Parkinson's Disease Clinical Trial
Official title:
Effects of Chocolate on Motor Symptoms of Parkinson's Disease - A Monocenter, Prospective, Observer-blinded Interventional Trial
Chocolate consumption has long been associated with enjoyment and pleasure. Popular claims
confer on chocolate the properties of being a stimulant, relaxant, euphoriant and
antidepressant. These possible pharmacological actions might be related to various biogenic
amines, such as serotonin, dopamine, tyramine, histamine, phenylethylamine and
cannabinoid-like substances. Most amines are metabolized by monoamineoxidase-A (MAO-A) and
are therefore unable to pass the blood-brain-barrier. In contrast, phenylethylamine is a
direct dopamine releasing ingredient and as a substrate of MAO-B and due to its lipophilic
structure even capable to pass the blood-brain-barrier. Within this line, own clinical
observations suggested an increased chocolate consumption in patients with Parkinson's
disease (PD) compared to healthy subjects and to their pre-disease state.
In a previous study, we assessed the consumption of chocolate and non-chocolate sweets in PD
patients and their partners (as household controls) using a self-questionnaire. Consumption
of chocolate was significantly higher in PD patients compared to controls, while consumption
of non-chocolate sweets was similar in both groups. Our study suggests that chocolate
consumption is increased in PD independent of concomitant depressive symptoms measured by
BDI-1. Although reasons for increased chocolate consumption in PD remain elusive, it may
hypothetically be a consequence of the high content of various biogenic amines as a content
of cocoa influencing dopamine metabolism.
Therefore, in the present study we aim to study the effects of dark chocolate with high
cocoa content (85%) compared to chocolate without any cocoa (white chocolate) on motor
symptoms in PD patients as measured with UPDRS part III (motor score). The principle design
of the intervention is similar to the standard pharmacological challenge test for studying
effects on motor symptoms in PD (e.g. levodopa challenge test).
n/a
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Single Blind (Investigator), Primary Purpose: Treatment
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