Parkinson's Disease Clinical Trial
Official title:
Modulation of Oxidative Stress and Apoptosis of Energy Metabolism by Deferiprone From the Circulating Lymphocytes of Patients With Parkinson's Disease or Amyotrophic Lateral Sclerosis
Peripheral blood mononuclear cells (PBMC) and platelets could be interesting ex vivo models
to study brain diseases. Indeed, there is no access to neurons from patients. However, PBMC
can exhibit different physiopathological mechanisms that are ubiquitous (i.e. oxidative
stress, mitochondriopathy with energy metabolism, inflammation, protein folding, iron
metabolism and programmed cell death ...). The platelets are pivotal in the healing system
with large range of growth factors. A new therapeutic concept of conservative iron chelation
with deferiprone for neuroprotection is under development.
The action of deferiprone on the different mechanisms and notably the oxidative stress are to
obtain from a collection of PBMC and platelets from patient having Parkinson's disease and
Amyotrophic lateral sclerosis and healthy controls to study ex vivo.
PBMC and platelets will be stored for future analyses.
The study collection of PBMC and platelets from 30 patient having Parkinson's disease 30
patients having Amyotrophic lateral sclerosis and 30 healthy controls.
The collection will be performed either by cytapheresis for half of the patient and by
collecting the whole blood for the other half.
PBMC and platelets will be stored at minus 80°C. PBMC of patients and controls are exposed ex
vivo to different pathological condition (mainly Hydrogen peroxide, menadione, hypoxia...)
with and without deferiprone to analyse whether the level of oxidative stress (Reactive
Oxygen Species and notably hydroxyl radical with hydroxypethidine probe with flow cytometry)
is reduced under deferiprone (primary criterion. Secondary analyses will concern the level of
iron, the energy metabolism (aerobic versus anaerobic and the level of Adenosine triphosphate
production), the type of cell death (apoptosis, autophagy and new programmed cell death:
Ferroptosis) and inflammation. Finally, the level of growth factors and their effectiveness
will be studied from platelets.
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