Conservative Iron Chelation as a Disease-modifying Strategy in Parkinson's Disease

Phase 2

Completed

• Conditions: Parkinson Disease
• Interventions: Drug: Placebo; Drug: Deferiprone

• Registration Number: NCT02655315
• Lead Sponsor: University Hospital, Lille

Brief Summary

This study evaluates the effect of iron chelation as a therapeutic strategy to slow the progression of Parkinson's disease. Half of participants will receive the deferiprone to 15 mg / kg twice daily morning and evening (30mg / kg per day), while the other half will receive a placebo. The treatment lasts nine months.

Detailed Description

This is the new concept of "conservative iron chelation". We recently demonstrated (for the first time) the feasibility, efficacy and acceptability of the conservative iron chelation approach in pilot translational studies in Parkinson's disease with a prototype drug: deferiprone (1,2-dimethyl-3-hydroxypyridin-4-one) (in the FAIR-PARK-I project led by the applicant and funded by French Ministry of Health). The only available blood-brain-barrier-permeable iron chelator deferiprone is approved for treating systemic iron overload in transfused patients with thalassemia. Deferiprone has been on the European Union market since 1999, with a favourable risk/benefit balance at dose of 75 to 100 mg/kg/day. The investigators shall adopt a repositioning strategy by using deferiprone at a lower dose of 30 mg/kg/day in this new indication for local iron overload in Parkinson's disease. Deferiprone will be the first-in-class drug for this novel therapeutic strategy. On the basis of the preclinical and clinical data from (FAIR-PARK-I), the present (FAIR-PARK-II) project should constitute a model for future cytoprotection strategies in neurodegenerative diseases; if deferiprone treatment is associated with significant slower disease progression, it would be the first non-dopaminergic drug to have a proven disease-modifying effect in Parkinson's disease.

Study Timeline

• Study First Submitted: 2016-01-07
• Study First Submitted QC: 2016-01-11
• Study First Posted: 2016-01-14
• Study Start: 2016-02-09
• Primary Completion: 2020-09-22
• Study Completion: 2020-09-22
• Status Verified: 2021-03
• Last Update Submitted: 2022-11-04
• Last Update Posted: 2022-11-07

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 372

Inclusion Criteria

1. Adult patients
2. Parkinson's disease diagnosed according United Kingdom Parkinson's disease Society Brain Bank Clinical Diagnostic Criteria and based on the presence of at least two of the three cardinal features of the disease (rest tremor, bradykinesia and rigidity). If rest tremor is not present, subjects must have unilateral onset of symptoms.
3. Treatment-naïve, i.e. the best population for assessing a disease-modifying effect without the interaction of dopaminergic treatment (no dopaminergic agonists, L-dopa, anticholinergics, monoamine oxidase B inhibitors (e.g. rasagiline) or deep brain stimulation).
4. Patients covered by a Health Insurance System in countries where required by law
5. Written informed consent dated and signed prior to the beginning of any procedures related to the clinical trial

Exclusion Criteria

1. Disease duration greater than 18 months.
2. Patients with high frequency of comorbidity or vital risks that may reasonably impair life expectancy
3. Subject with handicap required dopaminergic treatment at the inclusion and therefore likely not to bear 9 months without symptomatic treatment
4. Hoehn and Yahr stage 3 or more.
5. Significant cognitive impairment (a Mini Mental State Examination score <24 or an equivalent impairment on a similar scale) or dementia diagnosed in accordance with the Movement Disorders Society criteria (Emre et al., 2007).
6. Atypical or secondary parkinsonism (supranuclear palsy, multisystem atrophy, etc.) or anomalies on MRI suggestive of vascular involvement or significant cortical or subcortical atrophy (i.e. atypical for Parkinson's Disease).
7. Progressing axis I psychiatric disorders (psychosis, hallucinations, substance addiction, bipolar disorder, or severe depression), in accordance with the Diagnostic and Statistical Manual of Mental Disorders.
8. Subjects undergoing brain stimulation.
9. Positive Human Immunodepression Virus serology.
10. Hypersensitivity to deferiprone.
11. Patients with agranulocytosis or with a history of agranulocytosis.
12. Patients taking a treatment at risk of agranulocytosis (clozapine, Closaril®/Leponex®).
13. Patients with anaemia (regardless of the latter's aetiology) or a history of another haematological disease. Haemochromatosis is not an exclusion criterion.
14. Pregnant or breastfeeding women or women of childbearing potential not taking highly effective contraception.
15. Kidney or liver failure.
16. Other serious diseases.
17. Inability to provide informed consent.
18. Participation in another clinical trial with investigational medicinal product within 3 months prior to inclusion in the study
19. Patient who has suffered mild or moderate depressive episode and isn't in remission and on a stable medication for at least 8 weeks
20. Patient > 130k

Exclusion criteria for the biomarker study and the ancillary study (i) Magnetic Resonance Imaging:

• Subjects for whom Magnetic Resonance Imaging is contraindicated (metal objects in the body, severe claustrophobia, pacemaker, incompatible surgical material).
• Very severe rest tremor, which could induce Magnetic Resonance Imaging artefacts.

(ii) Lumbar puncture:

• Blood coagulation disorders, antiplatelet drugs or anticoagulants.
• Intracranial hypertension. (iii) Contraindications to nitrous oxide:
• Ventilation with Fraction of inspired Oxygen >50%, emphysema or pneumothorax
• Altered states of consciousness, non-cooperative patient (need to stop the nitrous oxide)

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
PLACEBO	Placebo	Half of participants will receive the placebo twice daily morning and evening. The treatment lasts nine months.
DEFERIPRONE	Deferiprone	Half of participants will receive the deferiprone (DFP) to 15 mg / kg twice daily morning and evening (30mg / kg per day).The treatment lasts nine months.

Primary Outcome Measures

Name	Time	Method
Global effect (symptomatic and disease modifying effects) on motor and non motor handicap	at 36 weeks	the change in the total Movement Disorders Society-Unified Parkinson Disease Rating Scale score between baseline and 36 weeks (i.e. the end of the placebo-controlled phase for analysis of both disease-modifying and symptomatic effects)

Secondary Outcome Measures

Name	Time	Method
Effect of the motor symptoms	baseline, at 12, 36 and 40 weeks	The effect of the motor symptoms will be analysed as the change in the subscale part III of the Movement Disorders Society-Unified Parkinson Disease Rating Scale score
Disease-modifying effect on motor and non motor handicap	baseline, at 40 weeks	It will be measured as the changes in the overall Movement Disorders Society-Unified Parkinson Disease Rating Scale score between baseline and week 40 (i.e. the end of the one-month post-treatment monitoring period), to analyse the disease-modifying effect without bias from the symptomatic effect of ongoing deferiprone treatment) on the study population
Effect on non-motor symptoms	baseline, at 12, 36 and 40 weeks	The effect on non motor symptoms will be analysed as the change in the subscale part I (cognition and behavior) of the Movement Disorders Society-Unified Parkinson Disease Rating Scale score
Effect on daily living	baseline, at 12, 36 and 40 weeks	The effect on daily living will be analysed as the change in the subscale part II (activities of daily living) of the Movement Disorders Society-Unified Parkinson Disease Rating Scale score
Quality of life and autonomy by PDQ-39 score	baseline, at 36 and 40 weeks	It will be analyzed as the change in the Parkinson's Disease Quality of Life (PDQ-39, via a 39-item self-questionnaire)
Health economics assessment	baseline, at 36 and 40 weeks	will be performed via a specific questionnaire provides a simple descriptive profile and a single index value for health status
Effect on overall cognitive status	baseline, at 12, 36 and 40 weeks	Measured by the score in the Montreal Cognitive Assessment
Effect on gait disorders	baseline, at 12, 36 and 40 weeks	Measured by the Stand Walk Sit test
Quality of life and autonomy by Clinical Global Impression score	baseline, at 36 and 40 weeks	the Clinical Global Impression scored by the examiner and the patient
Safety criteria	40 weeks	All the safety concerns will be listed in a table with the number of patients, the type the severity and the time of occurrence for; * adverse events; * neutropenia (weekly complete blood count); * agranulocytosis (weekly complete blood count); * anemia (weekly complete blood count); * iron metabolism abnormalities (haemoglobin, serum iron, ferritinemia, transferrin, total binding capacity, transferrin saturation coefficient, 24-hour urine iron).; * Standard biological abnormalities (fasting glucose, urea, creatinine, aspartate aminotransferase (AST), alanine aminotransferase (ALT) and (for all sexually active, fertile females) urine pregnancy tests.; * Abnormal physical examination (including vital signs, bodyweight, electrocardiogram and blood pressure)
EQ-5D questionnaire	baseline, at 36 and 40 weeks	the questionnaire provides a simple descriptive profile and a single index value for health status.
Lack of occurrence of motor fluctuations	baseline, at 12, 36 and 40 weeks	The lack of occurrence of motor fluctuations will be analysed on the subscale part IV of the Movement Disorders Society-Unified Parkinson Disease Rating Scale score

Trial Locations

Locations (25)

Centro Hospitalar e universitario de Coimbra; 🇵🇹 Coimbra, Portugal

Hôpital Wertheimer; 🇫🇷 Bron, France

Medizinische Universitat Innsbruck; 🇦🇹 Innsbruck, Austria

Univerzita Karlova V Praze; 🇨🇿 Prague, Czechia

CHU Pellegrin; 🇫🇷 Bordeaux, France

Charles University; 🇨🇿 Praha, Czechia

Hôpital Montpied; 🇫🇷 Clermont-Ferrand, France

Hôpital Salengro, CHRU; 🇫🇷 Lille, France

CHU la TIMONE; 🇫🇷 Marseille, France

AP-HP, Hôpital Pitié-Salpêtrière; 🇫🇷 Paris, France

CHU de Strasbourg, Hôpital de Hautepierre; 🇫🇷 Strasbourg, France

Chu Purpan; 🇫🇷 Toulouse, France

University Hospital, Saarland University; 🇩🇪 Homburg, Germany

Christian-albrechts universität zu kiel; 🇩🇪 Kiel, Germany

Acadamic central center, Amsterdam; 🇳🇱 Amsterdam, Netherlands

Klinik und Poliklinik für Neurologie der Universitätsmedizin Rostock; 🇩🇪 Rostock, Germany

Radboud university medical center; 🇳🇱 Nijmegen, Netherlands

Centro Hospitalar do Alto Ave; 🇵🇹 Guimarães, Portugal

Centro Hospitalar Lisboa Norte; 🇵🇹 Lisbon, Portugal

Hospital Clinic Universitari de Barcelona; 🇪🇸 Barcelona, Spain

Hospital de Bellvitge; 🇪🇸 Barcelona, Spain

Hospital de la Santa Creu i Sant Pau; 🇪🇸 Barcelona, Spain

Cambridge University Hospital; 🇬🇧 Cambridge, United Kingdom

University of Glasgow; 🇬🇧 Glasgow, United Kingdom

Newcastle University; 🇬🇧 Newcastle, United Kingdom