Trial of Deferiprone in Parkinson's Disease

David Devos; Julien Labreuche; Olivier Rascol; Jean-Christophe Corvol; Alain Duhamel; Pauline Guyon Delannoy; Werner Poewe; Yaroslau Compta; Nicola Pavese; EvÅen Ruzička; Petr Dušek; Bart Post; Bastiaan R. Bloem; Daniela Berg; Walter Maetzler; Markus Otto; Marie-Odile Habert; Stéphane Lehericy; Joaquim Ferreira; Richard Dodel; Christine Tranchant; Alexandre Eusebio; Stéphane Thobois; Ana-Raquel Marques; Wassilios G. Meissner; Fabienne Ory-Magne; Uwe Walter; Rob M. A. de Bie; Miguel Gago; Dolores Vilas; Jaime Kulisevsky; Cristina Januario; Miguel V. S. Coelho; Stefanie Behnke; Paul Worth; Klaus Seppi; Thavarak Ouk; Camille Potey; C. line Leclercq; Romain Viard; Gregory Kuchcinski; Renaud Lopes; Jean-Pierre Pruvo; Pascal Pigny; Guillaume Garçon; Ophélie Simonin; Jessica Carpentier; Anne-Sophie Rolland; Dag Nyholm; Christoph Scherfler; Jean-François Mangin; Marie Chupin; R. gis Bordet; David T. Dexter; Caroline Fradette; Michael Spino; Fernando Tricta; Scott Ayton; Ashley I. Bush; Jean-Christophe Devedjian; James A. Duce; Ioav Cabantchik; Luc Defebvre; Dominique Deplanque; Caroline Moreau

doi:https://doi.org/10.1056/NEJMoa2209254

Trial of Deferiprone in Parkinson's Disease

David Devos, Julien Labreuche, Olivier Rascol, Jean-Christophe Corvol, Alain Duhamel, Pauline Guyon Delannoy, Werner Poewe, Yaroslau Compta, Nicola Pavese, EvÅen Ruzička, Petr Dušek, Bart Post, Bastiaan R. Bloem, Daniela Berg, Walter Maetzler, Markus Otto, Marie-Odile Habert, Stéphane Lehericy, Joaquim Ferreira, Richard DodelChristine Tranchant, Alexandre Eusebio, Stéphane Thobois, Ana-Raquel Marques, Wassilios G. Meissner, Fabienne Ory-Magne, Uwe Walter, Rob M. A. de Bie, Miguel Gago, Dolores Vilas, Jaime Kulisevsky, Cristina Januario, Miguel V. S. Coelho, Stefanie Behnke, Paul Worth, Klaus Seppi, Thavarak Ouk, Camille Potey, C. line Leclercq, Romain Viard, Gregory Kuchcinski, Renaud Lopes, Jean-Pierre Pruvo, Pascal Pigny, Guillaume Garçon, Ophélie Simonin, Jessica Carpentier, Anne-Sophie Rolland, Dag Nyholm, Christoph Scherfler, Jean-François Mangin, Marie Chupin, R. gis Bordet, David T. Dexter, Caroline Fradette, Michael Spino, Fernando Tricta, Scott Ayton, Ashley I. Bush, Jean-Christophe Devedjian, James A. Duce, Ioav Cabantchik, Luc Defebvre, Dominique Deplanque, Caroline Moreau

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Abstract

Background Iron content is increased in the substantia nigra of persons with Parkinson's disease and may contribute to the pathophysiology of the disorder. Early research suggests that the iron chelator deferiprone can reduce nigrostriatal iron content in persons with Parkinson's disease, but its effects on disease progression are unclear. Methods We conducted a multicenter, phase 2, randomized, double-blind trial involving participants with newly diagnosed Parkinson's disease who had never received levodopa. Participants were assigned (in a 1:1 ratio) to receive oral deferiprone at a dose of 15 mg per kilogram of body weight twice daily or matched placebo for 36 weeks. Dopaminergic therapy was withheld unless deemed necessary for symptom control. The primary outcome was the change in the total score on the Movement Disorder Society-sponsored revision of the Unified Parkinson's Disease Rating Scale (MDS-UPDRS; range, 0 to 260, with higher scores indicating more severe impairment) at 36 weeks. Secondary and exploratory clinical outcomes at up to 40 weeks included measures of motor and nonmotor disability. Brain iron content measured with the use of magnetic resonance imaging was also an exploratory outcome. Results A total of 372 participants were enrolled; 186 were assigned to receive deferiprone and 186 to receive placebo. Progression of symptoms led to the initiation of dopaminergic therapy in 22.0% of the participants in the deferiprone group and 2.7% of those in the placebo group. The mean MDS-UPDRS total score at baseline was 34.3 in the deferiprone group and 33.2 in the placebo group and increased (worsened) by 15.6 points and 6.3 points, respectively (difference, 9.3 points; 95% confidence interval, 6.3 to 12.2; P<0.001). Nigrostriatal iron content decreased more in the deferiprone group than in the placebo group. The main serious adverse events with deferiprone were agranulocytosis in 2 participants and neutropenia in 3 participants. Conclusions In participants with early Parkinson's disease who had never received levodopa and in whom treatment with dopaminergic medications was not planned, deferiprone was associated with worse scores in measures of parkinsonism than those with placebo over a period of 36 weeks.

Original language	English
Pages (from-to)	2045-2055
Number of pages	11
Journal	New England journal of medicine
Volume	387
Issue number	22
DOIs	https://doi.org/10.1056/NEJMoa2209254
Publication status	Published - 1 Dec 2022

Keywords

Genetics
Geriatrics/Aging
Geriatrics/Aging General
Hematology/Oncology
Hematology/Oncology General
Neurology/Neurosurgery
Neuroscience
Parkinson Disease

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https://doi.org/10.1056/NEJMoa2209254

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Devos, D., Labreuche, J., Rascol, O., Corvol, J.-C., Duhamel, A., Delannoy, P. G., Poewe, W., Compta, Y., Pavese, N., Ruzička, E., Dušek, P., Post, B., Bloem, B. R., Berg, D., Maetzler, W., Otto, M., Habert, M.-O., Lehericy, S., Ferreira, J., ... Moreau, C. (2022). Trial of Deferiprone in Parkinson's Disease. New England journal of medicine, 387(22), 2045-2055. https://doi.org/10.1056/NEJMoa2209254

@article{b2c15915e1bf4049966af17c7997d6ab,

title = "Trial of Deferiprone in Parkinson's Disease",

abstract = "Background Iron content is increased in the substantia nigra of persons with Parkinson's disease and may contribute to the pathophysiology of the disorder. Early research suggests that the iron chelator deferiprone can reduce nigrostriatal iron content in persons with Parkinson's disease, but its effects on disease progression are unclear. Methods We conducted a multicenter, phase 2, randomized, double-blind trial involving participants with newly diagnosed Parkinson's disease who had never received levodopa. Participants were assigned (in a 1:1 ratio) to receive oral deferiprone at a dose of 15 mg per kilogram of body weight twice daily or matched placebo for 36 weeks. Dopaminergic therapy was withheld unless deemed necessary for symptom control. The primary outcome was the change in the total score on the Movement Disorder Society-sponsored revision of the Unified Parkinson's Disease Rating Scale (MDS-UPDRS; range, 0 to 260, with higher scores indicating more severe impairment) at 36 weeks. Secondary and exploratory clinical outcomes at up to 40 weeks included measures of motor and nonmotor disability. Brain iron content measured with the use of magnetic resonance imaging was also an exploratory outcome. Results A total of 372 participants were enrolled; 186 were assigned to receive deferiprone and 186 to receive placebo. Progression of symptoms led to the initiation of dopaminergic therapy in 22.0% of the participants in the deferiprone group and 2.7% of those in the placebo group. The mean MDS-UPDRS total score at baseline was 34.3 in the deferiprone group and 33.2 in the placebo group and increased (worsened) by 15.6 points and 6.3 points, respectively (difference, 9.3 points; 95% confidence interval, 6.3 to 12.2; P<0.001). Nigrostriatal iron content decreased more in the deferiprone group than in the placebo group. The main serious adverse events with deferiprone were agranulocytosis in 2 participants and neutropenia in 3 participants. Conclusions In participants with early Parkinson's disease who had never received levodopa and in whom treatment with dopaminergic medications was not planned, deferiprone was associated with worse scores in measures of parkinsonism than those with placebo over a period of 36 weeks.",

keywords = "Genetics, Geriatrics/Aging, Geriatrics/Aging General, Hematology/Oncology, Hematology/Oncology General, Neurology/Neurosurgery, Neuroscience, Parkinson Disease",

author = "David Devos and Julien Labreuche and Olivier Rascol and Jean-Christophe Corvol and Alain Duhamel and Delannoy, {Pauline Guyon} and Werner Poewe and Yaroslau Compta and Nicola Pavese and Ev{\AA}en Ruzi{\v c}ka and Petr Du{\v s}ek and Bart Post and Bloem, {Bastiaan R.} and Daniela Berg and Walter Maetzler and Markus Otto and Marie-Odile Habert and St{\'e}phane Lehericy and Joaquim Ferreira and Richard Dodel and Christine Tranchant and Alexandre Eusebio and St{\'e}phane Thobois and Ana-Raquel Marques and Meissner, {Wassilios G.} and Fabienne Ory-Magne and Uwe Walter and {de Bie}, {Rob M. A.} and Miguel Gago and Dolores Vilas and Jaime Kulisevsky and Cristina Januario and Coelho, {Miguel V. S.} and Stefanie Behnke and Paul Worth and Klaus Seppi and Thavarak Ouk and Camille Potey and Leclercq, {C. line} and Romain Viard and Gregory Kuchcinski and Renaud Lopes and Jean-Pierre Pruvo and Pascal Pigny and Guillaume Gar{\c c}on and Oph{\'e}lie Simonin and Jessica Carpentier and Anne-Sophie Rolland and Dag Nyholm and Christoph Scherfler and Jean-Fran{\c c}ois Mangin and Marie Chupin and Bordet, {R. gis} and Dexter, {David T.} and Caroline Fradette and Michael Spino and Fernando Tricta and Scott Ayton and Bush, {Ashley I.} and Jean-Christophe Devedjian and Duce, {James A.} and Ioav Cabantchik and Luc Defebvre and Dominique Deplanque and Caroline Moreau",

note = "Funding Information: This was an investigator-initiated, multicenter, international trial conducted at 23 sites (see the , available with the full text of this article at NEJM.org). The trial was supported by the European Union Horizon 2020 funding program, through the FAIR PARK II network (www.fairpark2.eu), with the support of the French NS-Park/FCRIN network ( https://parkinson.network/en ), in collaboration with ApoPharma and Chiesi, which provided deferiprone and placebo but otherwise had no role in the design of the trial, the analysis or interpretation of the data, the writing of the manuscript, or the decision to submit the manuscript for publication. The first and last authors were primarily responsible for writing the initial manuscript. An independent data and safety monitoring board reviewed safety data throughout the trial. Statistical analyses were independently performed by members of the Department of Biostatistics, Lille University Hospital, France (second and fifth authors). All the authors vouch for the completeness and accuracy of the data, the adherence of the trial to the (available at NEJM.org), and the reporting of all adverse events. Funding Information: Supported by a grant (633190) from the European Union Horizon 2020 research and innovation program to the FAIR PARK II project. Publisher Copyright: {\textcopyright} 2022 Massachusetts Medical Society.",

year = "2022",

month = dec,

day = "1",

doi = "https://doi.org/10.1056/NEJMoa2209254",

language = "English",

volume = "387",

pages = "2045--2055",

journal = "New England journal of medicine",

issn = "0028-4793",

publisher = "Massachussetts Medical Society",

number = "22",

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Devos, D, Labreuche, J, Rascol, O, Corvol, J-C, Duhamel, A, Delannoy, PG, Poewe, W, Compta, Y, Pavese, N, Ruzička, E, Dušek, P, Post, B, Bloem, BR, Berg, D, Maetzler, W, Otto, M, Habert, M-O, Lehericy, S, Ferreira, J, Dodel, R, Tranchant, C, Eusebio, A, Thobois, S, Marques, A-R, Meissner, WG, Ory-Magne, F, Walter, U, de Bie, RMA, Gago, M, Vilas, D, Kulisevsky, J, Januario, C, Coelho, MVS, Behnke, S, Worth, P, Seppi, K, Ouk, T, Potey, C, Leclercq, CL, Viard, R, Kuchcinski, G, Lopes, R, Pruvo, J-P, Pigny, P, Garçon, G, Simonin, O, Carpentier, J, Rolland, A-S, Nyholm, D, Scherfler, C, Mangin, J-F, Chupin, M, Bordet, RG, Dexter, DT, Fradette, C, Spino, M, Tricta, F, Ayton, S, Bush, AI, Devedjian, J-C, Duce, JA, Cabantchik, I, Defebvre, L, Deplanque, D & Moreau, C 2022, 'Trial of Deferiprone in Parkinson's Disease', New England journal of medicine, vol. 387, no. 22, pp. 2045-2055. https://doi.org/10.1056/NEJMoa2209254

TY - JOUR

T1 - Trial of Deferiprone in Parkinson's Disease

AU - Devos, David

AU - Labreuche, Julien

AU - Rascol, Olivier

AU - Corvol, Jean-Christophe

AU - Duhamel, Alain

AU - Delannoy, Pauline Guyon

AU - Poewe, Werner

AU - Compta, Yaroslau

AU - Pavese, Nicola

AU - Ruzička, EvÅen

AU - Dušek, Petr

AU - Post, Bart

AU - Bloem, Bastiaan R.

AU - Berg, Daniela

AU - Maetzler, Walter

AU - Otto, Markus

AU - Habert, Marie-Odile

AU - Lehericy, Stéphane

AU - Ferreira, Joaquim

AU - Dodel, Richard

AU - Tranchant, Christine

AU - Eusebio, Alexandre

AU - Thobois, Stéphane

AU - Marques, Ana-Raquel

AU - Meissner, Wassilios G.

AU - Ory-Magne, Fabienne

AU - Walter, Uwe

AU - de Bie, Rob M. A.

AU - Gago, Miguel

AU - Vilas, Dolores

AU - Kulisevsky, Jaime

AU - Januario, Cristina

AU - Coelho, Miguel V. S.

AU - Behnke, Stefanie

AU - Worth, Paul

AU - Seppi, Klaus

AU - Ouk, Thavarak

AU - Potey, Camille

AU - Leclercq, C. line

AU - Viard, Romain

AU - Kuchcinski, Gregory

AU - Lopes, Renaud

AU - Pruvo, Jean-Pierre

AU - Pigny, Pascal

AU - Garçon, Guillaume

AU - Simonin, Ophélie

AU - Carpentier, Jessica

AU - Rolland, Anne-Sophie

AU - Nyholm, Dag

AU - Scherfler, Christoph

AU - Mangin, Jean-François

AU - Chupin, Marie

AU - Bordet, R. gis

AU - Dexter, David T.

AU - Fradette, Caroline

AU - Spino, Michael

AU - Tricta, Fernando

AU - Ayton, Scott

AU - Bush, Ashley I.

AU - Devedjian, Jean-Christophe

AU - Duce, James A.

AU - Cabantchik, Ioav

AU - Defebvre, Luc

AU - Deplanque, Dominique

AU - Moreau, Caroline

N1 - Funding Information: This was an investigator-initiated, multicenter, international trial conducted at 23 sites (see the , available with the full text of this article at NEJM.org). The trial was supported by the European Union Horizon 2020 funding program, through the FAIR PARK II network (www.fairpark2.eu), with the support of the French NS-Park/FCRIN network ( https://parkinson.network/en ), in collaboration with ApoPharma and Chiesi, which provided deferiprone and placebo but otherwise had no role in the design of the trial, the analysis or interpretation of the data, the writing of the manuscript, or the decision to submit the manuscript for publication. The first and last authors were primarily responsible for writing the initial manuscript. An independent data and safety monitoring board reviewed safety data throughout the trial. Statistical analyses were independently performed by members of the Department of Biostatistics, Lille University Hospital, France (second and fifth authors). All the authors vouch for the completeness and accuracy of the data, the adherence of the trial to the (available at NEJM.org), and the reporting of all adverse events. Funding Information: Supported by a grant (633190) from the European Union Horizon 2020 research and innovation program to the FAIR PARK II project. Publisher Copyright: © 2022 Massachusetts Medical Society.

PY - 2022/12/1

Y1 - 2022/12/1

N2 - Background Iron content is increased in the substantia nigra of persons with Parkinson's disease and may contribute to the pathophysiology of the disorder. Early research suggests that the iron chelator deferiprone can reduce nigrostriatal iron content in persons with Parkinson's disease, but its effects on disease progression are unclear. Methods We conducted a multicenter, phase 2, randomized, double-blind trial involving participants with newly diagnosed Parkinson's disease who had never received levodopa. Participants were assigned (in a 1:1 ratio) to receive oral deferiprone at a dose of 15 mg per kilogram of body weight twice daily or matched placebo for 36 weeks. Dopaminergic therapy was withheld unless deemed necessary for symptom control. The primary outcome was the change in the total score on the Movement Disorder Society-sponsored revision of the Unified Parkinson's Disease Rating Scale (MDS-UPDRS; range, 0 to 260, with higher scores indicating more severe impairment) at 36 weeks. Secondary and exploratory clinical outcomes at up to 40 weeks included measures of motor and nonmotor disability. Brain iron content measured with the use of magnetic resonance imaging was also an exploratory outcome. Results A total of 372 participants were enrolled; 186 were assigned to receive deferiprone and 186 to receive placebo. Progression of symptoms led to the initiation of dopaminergic therapy in 22.0% of the participants in the deferiprone group and 2.7% of those in the placebo group. The mean MDS-UPDRS total score at baseline was 34.3 in the deferiprone group and 33.2 in the placebo group and increased (worsened) by 15.6 points and 6.3 points, respectively (difference, 9.3 points; 95% confidence interval, 6.3 to 12.2; P<0.001). Nigrostriatal iron content decreased more in the deferiprone group than in the placebo group. The main serious adverse events with deferiprone were agranulocytosis in 2 participants and neutropenia in 3 participants. Conclusions In participants with early Parkinson's disease who had never received levodopa and in whom treatment with dopaminergic medications was not planned, deferiprone was associated with worse scores in measures of parkinsonism than those with placebo over a period of 36 weeks.

AB - Background Iron content is increased in the substantia nigra of persons with Parkinson's disease and may contribute to the pathophysiology of the disorder. Early research suggests that the iron chelator deferiprone can reduce nigrostriatal iron content in persons with Parkinson's disease, but its effects on disease progression are unclear. Methods We conducted a multicenter, phase 2, randomized, double-blind trial involving participants with newly diagnosed Parkinson's disease who had never received levodopa. Participants were assigned (in a 1:1 ratio) to receive oral deferiprone at a dose of 15 mg per kilogram of body weight twice daily or matched placebo for 36 weeks. Dopaminergic therapy was withheld unless deemed necessary for symptom control. The primary outcome was the change in the total score on the Movement Disorder Society-sponsored revision of the Unified Parkinson's Disease Rating Scale (MDS-UPDRS; range, 0 to 260, with higher scores indicating more severe impairment) at 36 weeks. Secondary and exploratory clinical outcomes at up to 40 weeks included measures of motor and nonmotor disability. Brain iron content measured with the use of magnetic resonance imaging was also an exploratory outcome. Results A total of 372 participants were enrolled; 186 were assigned to receive deferiprone and 186 to receive placebo. Progression of symptoms led to the initiation of dopaminergic therapy in 22.0% of the participants in the deferiprone group and 2.7% of those in the placebo group. The mean MDS-UPDRS total score at baseline was 34.3 in the deferiprone group and 33.2 in the placebo group and increased (worsened) by 15.6 points and 6.3 points, respectively (difference, 9.3 points; 95% confidence interval, 6.3 to 12.2; P<0.001). Nigrostriatal iron content decreased more in the deferiprone group than in the placebo group. The main serious adverse events with deferiprone were agranulocytosis in 2 participants and neutropenia in 3 participants. Conclusions In participants with early Parkinson's disease who had never received levodopa and in whom treatment with dopaminergic medications was not planned, deferiprone was associated with worse scores in measures of parkinsonism than those with placebo over a period of 36 weeks.

KW - Genetics

KW - Geriatrics/Aging

KW - Geriatrics/Aging General

KW - Hematology/Oncology

KW - Hematology/Oncology General

KW - Neurology/Neurosurgery

KW - Neuroscience

KW - Parkinson Disease

UR - http://www.scopus.com/inward/record.url?scp=85145500633&partnerID=8YFLogxK

U2 - https://doi.org/10.1056/NEJMoa2209254

DO - https://doi.org/10.1056/NEJMoa2209254

M3 - Article

C2 - 36449420

SN - 0028-4793

VL - 387

SP - 2045

EP - 2055

JO - New England journal of medicine

JF - New England journal of medicine

IS - 22

ER -

Trial of Deferiprone in Parkinson's Disease

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