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A Double-Blind, Delayed-Start Trial of Rasagiline in Parkinson's Disease

Identifieur interne : 000779 ( PascalFrancis/Curation ); précédent : 000778; suivant : 000780

A Double-Blind, Delayed-Start Trial of Rasagiline in Parkinson's Disease

Auteurs : C. Warren Olanow [États-Unis] ; Olivier Rascol [France] ; Robert Hauser [États-Unis] ; Paul D. Feigin [Israël] ; Joseph Jankovic [États-Unis] ; Anthony Lang [Canada] ; William Langston [États-Unis] ; Eldad Melamed [Israël] ; Werner Poewe [Autriche] ; Fabrizio Stocchi [Italie] ; Eduardo Tolosa [Espagne]

Source :

RBID : Pascal:09-0410176

Descripteurs français

English descriptors

Abstract

BACKGROUND A therapy that slows disease progression is the major unmet need in Parkinson's disease. METHODS In this double-blind trial, we examined the possibility that rasagiline has disease-modifying effects in Parkinson's disease. A total of 1176 subjects with untreated Parkinson's disease were randomly assigned to receive rasagiline (at a dose of either 1 mg or 2 mg per day) for 72 weeks (the early-start group) or placebo for 36 weeks followed by rasagiline (at a dose of either 1 mg or 2 mg per day) for 36 weeks (the delayed-start group). To determine a positive result with either dose, the early-start treatment group had to meet each of three hierarchical end points of the primary analysis based on the Unified Parkinson's Disease Rating Scale (UPDRS, a 176-point scale, with higher numbers indicating more severe disease): superiority to placebo in the rate of change in the UPDRS score between weeks 12 and 36, superiority to delayed-start treatment in the change in the score between baseline and week 72, and noninferiority to delayed-start treatment in the rate of change in the score between weeks 48 and 72. RESULTS Early-start treatment with rasagiline at a dose of 1 mg per day met all end points in the primary analysis: a smaller mean (±SE) increase (rate of worsening) in the UPDRS score between weeks 12 and 36 (0.09±0.02 points per week in the early-start group vs. 0.14±0.01 points per week in the placebo group, P=0.01), less worsening in the score between baseline and week 72 (2.82±0.53 points in the early-start group vs. 4.52±0.5G points in the delayed-start group, P=0.02), and noninferiority between the two groups with respect to the rate of change in the UPDRS score between weeks 48 and 72 (0.085±0.02 points per week in the early-start group vs. 0.085±0.02 points per week in the delayed-start group, P<0.001). All three end points were not met with rasagiline at a dose of 2 mg per day, since the change in the UPDRS score between baseline and week 72 was not significantly different in the two groups (3.47±0.50 points in the early-start group and 3.11±0.50 points in the delayed-start group, P=0.60). CONCLUSIONS Early treatment with rasagiline at a dose of 1 mg per day provided benefits that were consistent with a possible disease-modifying effect, but early treatment with rasagiline at a dose of 2 mg per day did not. Because the two doses were associated with different outcomes, the study results must be interpreted with caution. (ClinicalTrials. gov number, NCT00256204.).
pA  
A01 01  1    @0 0028-4793
A02 01      @0 NEJMAG
A03   1    @0 N. Engl. j. med.
A05       @2 361
A06       @2 13
A08 01  1  ENG  @1 A Double-Blind, Delayed-Start Trial of Rasagiline in Parkinson's Disease
A11 01  1    @1 OLANOW (C. Warren)
A11 02  1    @1 RASCOL (Olivier)
A11 03  1    @1 HAUSER (Robert)
A11 04  1    @1 FEIGIN (Paul D.)
A11 05  1    @1 JANKOVIC (Joseph)
A11 06  1    @1 LANG (Anthony)
A11 07  1    @1 LANGSTON (William)
A11 08  1    @1 MELAMED (Eldad)
A11 09  1    @1 POEWE (Werner)
A11 10  1    @1 STOCCHI (Fabrizio)
A11 11  1    @1 TOLOSA (Eduardo)
A14 01      @1 Department of Neurology and Neuroscience, Mount Sinai School of Medicine @2 New York @3 USA @Z 1 aut.
A14 02      @1 INSERM CIC-9302 and UMR-825, Departments of Clinical Pharmacology and Neurosciences, Centre Hospitalier Universitaire and University of Toulouse, Faculty of Medicine @2 Toulouse @3 FRA @Z 2 aut.
A14 03      @1 Department of Neurology, University of South Florida @2 Tampa @3 USA @Z 3 aut.
A14 04      @1 Department of Industrial Engineering and Management, Technion-Israel Institute of Technology @2 Haifa @3 ISR @Z 4 aut.
A14 05      @1 Department of Neurology, Baylor College of Medicine @2 Houston @3 USA @Z 5 aut.
A14 06      @1 Division of Neurology, University of Toronto @2 Toronto @3 CAN @Z 6 aut.
A14 07      @1 California Parkinson Institute @2 Sunnyvale @3 USA @Z 7 aut.
A14 08      @1 Department of Neurology, Rabin Medical Center, Beilinson Campus @2 Petah Tikva @3 ISR @Z 8 aut.
A14 09      @1 Sackler School of Medicine @2 Tel Aviv @3 ISR @Z 8 aut.
A14 10      @1 Department of Neurology, Innsbruck Medical University @2 Innsbruck @3 AUT @Z 9 aut.
A14 11      @1 Institute of Neurology, Istituto di Ricovero e Cura a Carattere Scientifico San Raffaele Pisana @2 Rome @3 ITA @Z 10 aut.
A14 12      @1 Department of Neurology, University of Barcelona @2 Barcelona @3 ESP @Z 11 aut.
A14 13      @1 Centro de Investigacíon Biomédica en Red Sobre Enfermedades Neurodegenerativas @2 Madrid @3 ESP @Z 11 aut.
A17 01  1    @1 ADAGIO Study Investigators @3 INC
A20       @1 1268-1278
A21       @1 2009
A23 01      @0 ENG
A43 01      @1 INIST @2 6013 @5 354000171975430070
A44       @0 0000 @1 © 2009 INIST-CNRS. All rights reserved.
A45       @0 27 ref.
A47 01  1    @0 09-0410176
A60       @1 P
A61       @0 A
A64 01  1    @0 The New England journal of medicine
A66 01      @0 USA
C01 01    ENG  @0 BACKGROUND A therapy that slows disease progression is the major unmet need in Parkinson's disease. METHODS In this double-blind trial, we examined the possibility that rasagiline has disease-modifying effects in Parkinson's disease. A total of 1176 subjects with untreated Parkinson's disease were randomly assigned to receive rasagiline (at a dose of either 1 mg or 2 mg per day) for 72 weeks (the early-start group) or placebo for 36 weeks followed by rasagiline (at a dose of either 1 mg or 2 mg per day) for 36 weeks (the delayed-start group). To determine a positive result with either dose, the early-start treatment group had to meet each of three hierarchical end points of the primary analysis based on the Unified Parkinson's Disease Rating Scale (UPDRS, a 176-point scale, with higher numbers indicating more severe disease): superiority to placebo in the rate of change in the UPDRS score between weeks 12 and 36, superiority to delayed-start treatment in the change in the score between baseline and week 72, and noninferiority to delayed-start treatment in the rate of change in the score between weeks 48 and 72. RESULTS Early-start treatment with rasagiline at a dose of 1 mg per day met all end points in the primary analysis: a smaller mean (±SE) increase (rate of worsening) in the UPDRS score between weeks 12 and 36 (0.09±0.02 points per week in the early-start group vs. 0.14±0.01 points per week in the placebo group, P=0.01), less worsening in the score between baseline and week 72 (2.82±0.53 points in the early-start group vs. 4.52±0.5G points in the delayed-start group, P=0.02), and noninferiority between the two groups with respect to the rate of change in the UPDRS score between weeks 48 and 72 (0.085±0.02 points per week in the early-start group vs. 0.085±0.02 points per week in the delayed-start group, P<0.001). All three end points were not met with rasagiline at a dose of 2 mg per day, since the change in the UPDRS score between baseline and week 72 was not significantly different in the two groups (3.47±0.50 points in the early-start group and 3.11±0.50 points in the delayed-start group, P=0.60). CONCLUSIONS Early treatment with rasagiline at a dose of 1 mg per day provided benefits that were consistent with a possible disease-modifying effect, but early treatment with rasagiline at a dose of 2 mg per day did not. Because the two doses were associated with different outcomes, the study results must be interpreted with caution. (ClinicalTrials. gov number, NCT00256204.).
C02 01  X    @0 002B01
C02 02  X    @0 002B17G
C02 03  X    @0 002B18C13
C03 01  X  FRE  @0 Rasagiline @2 NK @2 FR @5 01
C03 01  X  ENG  @0 Rasagiline @2 NK @2 FR @5 01
C03 01  X  SPA  @0 Rasagilina @2 NK @2 FR @5 01
C03 02  X  FRE  @0 Etude double insu @5 02
C03 02  X  ENG  @0 Double blind study @5 02
C03 02  X  SPA  @0 Estudio doble ciego @5 02
C03 03  X  FRE  @0 Retard @5 03
C03 03  X  ENG  @0 Delay @5 03
C03 03  X  SPA  @0 Retraso @5 03
C03 04  X  FRE  @0 Maladie de Parkinson @2 NM @5 04
C03 04  X  ENG  @0 Parkinson disease @2 NM @5 04
C03 04  X  SPA  @0 Parkinson enfermedad @2 NM @5 04
C03 05  X  FRE  @0 Médecine @5 05
C03 05  X  ENG  @0 Medicine @5 05
C03 05  X  SPA  @0 Medicina @5 05
C03 06  X  FRE  @0 Antiparkinsonien @5 25
C03 06  X  ENG  @0 Antiparkinson agent @5 25
C03 06  X  SPA  @0 Antiparkinsoniano @5 25
C07 01  X  FRE  @0 Inhibiteur de la monoamine oxidase B @5 37
C07 01  X  ENG  @0 Monoamine oxidase B inhibitor @5 37
C07 01  X  SPA  @0 Inhibidor monoamine oxidase B @5 37
C07 02  X  FRE  @0 Pathologie de l'encéphale @5 38
C07 02  X  ENG  @0 Cerebral disorder @5 38
C07 02  X  SPA  @0 Encéfalo patología @5 38
C07 03  X  FRE  @0 Syndrome extrapyramidal @5 39
C07 03  X  ENG  @0 Extrapyramidal syndrome @5 39
C07 03  X  SPA  @0 Extrapiramidal síndrome @5 39
C07 04  X  FRE  @0 Maladie dégénérative @5 40
C07 04  X  ENG  @0 Degenerative disease @5 40
C07 04  X  SPA  @0 Enfermedad degenerativa @5 40
C07 05  X  FRE  @0 Pathologie du système nerveux central @5 41
C07 05  X  ENG  @0 Central nervous system disease @5 41
C07 05  X  SPA  @0 Sistema nervosio central patología @5 41
C07 06  X  FRE  @0 Pathologie du système nerveux @5 42
C07 06  X  ENG  @0 Nervous system diseases @5 42
C07 06  X  SPA  @0 Sistema nervioso patología @5 42
N21       @1 299
N44 01      @1 OTO
N82       @1 OTO

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Pascal:09-0410176

Le document en format XML

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<name sortKey="Jankovic, Joseph" sort="Jankovic, Joseph" uniqKey="Jankovic J" first="Joseph" last="Jankovic">Joseph Jankovic</name>
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<name sortKey="Lang, Anthony" sort="Lang, Anthony" uniqKey="Lang A" first="Anthony" last="Lang">Anthony Lang</name>
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<name sortKey="Langston, William" sort="Langston, William" uniqKey="Langston W" first="William" last="Langston">William Langston</name>
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<s1>California Parkinson Institute</s1>
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<country>États-Unis</country>
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<name sortKey="Melamed, Eldad" sort="Melamed, Eldad" uniqKey="Melamed E" first="Eldad" last="Melamed">Eldad Melamed</name>
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<inist:fA14 i1="09">
<s1>Sackler School of Medicine</s1>
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<s3>ISR</s3>
<sZ>8 aut.</sZ>
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<country>Israël</country>
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<name sortKey="Poewe, Werner" sort="Poewe, Werner" uniqKey="Poewe W" first="Werner" last="Poewe">Werner Poewe</name>
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<country>Autriche</country>
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<name sortKey="Stocchi, Fabrizio" sort="Stocchi, Fabrizio" uniqKey="Stocchi F" first="Fabrizio" last="Stocchi">Fabrizio Stocchi</name>
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<s1>Institute of Neurology, Istituto di Ricovero e Cura a Carattere Scientifico San Raffaele Pisana</s1>
<s2>Rome</s2>
<s3>ITA</s3>
<sZ>10 aut.</sZ>
</inist:fA14>
<country>Italie</country>
</affiliation>
</author>
<author>
<name sortKey="Tolosa, Eduardo" sort="Tolosa, Eduardo" uniqKey="Tolosa E" first="Eduardo" last="Tolosa">Eduardo Tolosa</name>
<affiliation wicri:level="1">
<inist:fA14 i1="12">
<s1>Department of Neurology, University of Barcelona</s1>
<s2>Barcelona</s2>
<s3>ESP</s3>
<sZ>11 aut.</sZ>
</inist:fA14>
<country>Espagne</country>
</affiliation>
<affiliation wicri:level="1">
<inist:fA14 i1="13">
<s1>Centro de Investigacíon Biomédica en Red Sobre Enfermedades Neurodegenerativas</s1>
<s2>Madrid</s2>
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<title level="j" type="main">The New England journal of medicine</title>
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<idno type="ISSN">0028-4793</idno>
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<term>Antiparkinson agent</term>
<term>Delay</term>
<term>Double blind study</term>
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<term>Parkinson disease</term>
<term>Rasagiline</term>
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<term>Rasagiline</term>
<term>Etude double insu</term>
<term>Retard</term>
<term>Maladie de Parkinson</term>
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<div type="abstract" xml:lang="en">BACKGROUND A therapy that slows disease progression is the major unmet need in Parkinson's disease. METHODS In this double-blind trial, we examined the possibility that rasagiline has disease-modifying effects in Parkinson's disease. A total of 1176 subjects with untreated Parkinson's disease were randomly assigned to receive rasagiline (at a dose of either 1 mg or 2 mg per day) for 72 weeks (the early-start group) or placebo for 36 weeks followed by rasagiline (at a dose of either 1 mg or 2 mg per day) for 36 weeks (the delayed-start group). To determine a positive result with either dose, the early-start treatment group had to meet each of three hierarchical end points of the primary analysis based on the Unified Parkinson's Disease Rating Scale (UPDRS, a 176-point scale, with higher numbers indicating more severe disease): superiority to placebo in the rate of change in the UPDRS score between weeks 12 and 36, superiority to delayed-start treatment in the change in the score between baseline and week 72, and noninferiority to delayed-start treatment in the rate of change in the score between weeks 48 and 72. RESULTS Early-start treatment with rasagiline at a dose of 1 mg per day met all end points in the primary analysis: a smaller mean (±SE) increase (rate of worsening) in the UPDRS score between weeks 12 and 36 (0.09±0.02 points per week in the early-start group vs. 0.14±0.01 points per week in the placebo group, P=0.01), less worsening in the score between baseline and week 72 (2.82±0.53 points in the early-start group vs. 4.52±0.5G points in the delayed-start group, P=0.02), and noninferiority between the two groups with respect to the rate of change in the UPDRS score between weeks 48 and 72 (0.085±0.02 points per week in the early-start group vs. 0.085±0.02 points per week in the delayed-start group, P<0.001). All three end points were not met with rasagiline at a dose of 2 mg per day, since the change in the UPDRS score between baseline and week 72 was not significantly different in the two groups (3.47±0.50 points in the early-start group and 3.11±0.50 points in the delayed-start group, P=0.60). CONCLUSIONS Early treatment with rasagiline at a dose of 1 mg per day provided benefits that were consistent with a possible disease-modifying effect, but early treatment with rasagiline at a dose of 2 mg per day did not. Because the two doses were associated with different outcomes, the study results must be interpreted with caution. (ClinicalTrials. gov number, NCT00256204.).</div>
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