Safety and efficacy of pridopidine in patients with Huntington's disease (PRIDE-HD): a phase 2, randomised, placebo-controlled, multicentre, dose-ranging study

European Huntington's Disease Network; Huntington Study Group investigators

doi:10.1016/S1474-4422(18)30391-0

Safety and efficacy of pridopidine in patients with Huntington's disease (PRIDE-HD): a phase 2, randomised, placebo-controlled, multicentre, dose-ranging study

European Huntington's Disease Network, Huntington Study Group investigators

Vagelos College of Physicians and Surgeons

Producción científica › revisión exhaustiva

79 Citas (Scopus)

Resumen

Background: Previous trials have shown that pridopidine might reduce motor impairment in patients with Huntington's disease. The aim of this study was to ascertain whether higher doses of pridopidine than previously tested reduce motor symptoms in a dose-dependent manner while maintaining acceptable safety and tolerability. Methods: PRIDE-HD was a randomised, placebo-controlled, phase 2, dose-ranging study in adults (aged ≥21 years) with Huntington's disease at outpatient clinics in 53 sites across 12 countries (Australia, Austria, Canada, Denmark, France, Germany, Italy, Poland, Russia, the Netherlands, the UK, and the USA). Eligible patients had clinical onset after age 18 years, 36 or more cytosine-adenine-guanine repeats in the huntingtin gene, motor symptoms (Unified Huntington's Disease Rating Scale total motor score [UHDRS-TMS] ≥25 points), and reduced independence (UHDRS independence score ≤90%). Patients were randomly assigned (1:1:1:1:1) with centralised interactive-response technology to receive one of four doses of pridopidine (45, 67·5, 90, or 112·5 mg) or placebo orally twice a day for 52 weeks. Randomisation was stratified within centres by neuroleptic drug use. The primary efficacy endpoint was change in the UHDRS-TMS from baseline to 26 weeks, which was assessed in all randomised patients who received at least one dose of study drug and had at least one post-baseline efficacy assessment (full analysis set). Participants and investigators were masked to treatment assignment. This trial is registered with EudraCT (2013-001888-23) and ClinicalTrials.gov (NCT02006472). Findings: Between Feb 13, 2014, and July 5, 2016, 408 patients were enrolled and randomly assigned to receive placebo (n=82) or pridopidine 45 mg (n=81), 67·5 mg (n=82), 90 mg (n=81), or 112·5 mg (n=82) twice daily for 26 weeks. The full analysis set included 397 patients (81 in the placebo group, 75 in the 45 mg group, 79 in the 67·5 mg group, 81 in the 90 mg group, and 81 in the 112·5 mg group). Pridopidine did not significantly change the UHDRS-TMS at 26 weeks compared with placebo at any dose. The most frequent adverse events across all groups were diarrhoea, vomiting, nasopharyngitis, falls, headache, insomnia, and anxiety. The most common treatment-related adverse events were insomnia, diarrhoea, nausea, and dizziness. Serious adverse events occurred in the pridopidine groups only and were most frequently falls (n=5), suicide attempt (n=4), suicidal ideation (n=3), head injury (n=3), and aspiration pneumonia (n=3). No new safety or tolerability concerns emerged in this study. One death in the pridopidine 112·5 mg group due to aspiration pneumonia was considered to be possibly related to the study drug. Interpretation: Pridopidine did not improve the UHDRS-TMS at week 26 compared with placebo and, thus, the results of secondary or tertiary analyses in previous trials were not replicated. A potentially strong placebo effect needs to be ruled out in future studies. Funding: Teva Pharmaceutical Industries.

Idioma original	English
Páginas (desde-hasta)	165-176
Número de páginas	12
Publicación	The Lancet Neurology
Volumen	18
N.º	2
DOI	https://doi.org/10.1016/S1474-4422(18)30391-0
Estado	Published - feb. 2019

Financiación

RR is founding director and owner of the George Huntington Institute, a private research institute focused on clinical and preclinical research in Huntington's disease, and QuantiMedis, a clinical research organisation providing Q-Motor services in clinical trials and research. He serves as an elected member of the steering committees of the EHDN and the HSG, co-chair of the Task Force on Huntington's Disease, and member of the Task Force on Technology of the International Parkinson and Movement Disorder Society. He has provided consulting services, advisory board functions, clinical trial services, Q-Motor analyses, or lectures for Actelion Pharmaceuticals, Amarin Neuroscience, AOP Orphan Pharmaceuticals, Cure Huntington Disease Initiative Foundation (CHDI), Desitin, Hoffmann-La Roche, Ionis Pharmaceuticals, Ipsen, Lundbeck, Link Medicine, Meda Pharma, Medivation, Mitoconix, Neurocrine Biosciences, Neurosearch, Novartis, Omeros, Pfizer, Prana Biotechnology, Prilenia Therapeutics, Raptor Pharmaceuticals, Siena Biotech, Temmler Pharma, Teva Pharmaceuticals, uniQure, Vaccinex, Wave Life Sciences, and Wyeth Pharmaceuticals. He has received grant support from Bundesministerium für Bildung und Forschung (BMBF), CHDI, Deutsche Forschungsgemeinschaft (DFG), Deutsches Zentrum für Neurodegeneration und Entzündung, European Union Seventh Framework Program (EU-FP7), EHDN, High Q Foundation, and National Science Foundation. AM has received grant support from, and participated on advisory boards and lectured for, Teva Pharmaceuticals. NG and J-MS are employed by Teva Pharmaceuticals. RS is an employee of the George Huntington Institute and received funding from the EU-FP7 for the further development of Q-Motor measures for clinical trial use. FS provided consulting and participated on advisory boards for Teva Pharmaceuticals, Pfizer, Raptor, Omani Ministry of Health, and Istituto per la Sicurezza Sociale di San Marino. He is co-founder of, and scientific officer and consultant for, the not-for-profit organisation Italian League for Research on Huntington and related diseases. BB, EE, IDG, ATW, SP, and MH were employed by Teva Pharmaceuticals at the time of study and manuscript preparation. SP has patents pending for use of pridopidine to treat dystonias and functional decline. KK has received consulting fees from Acorda, Astellas Pharma, AstraZeneca, BioMarin Pharmaceutica, Biotie, Britannia, CHDI, Clearpoint Strategy Group, Clintrex, Corium International, Cynapsus, Forward Pharma, Genzyme, INC Research, Intec, Lundbeck, Medivation, Melior Discovery, Neuroderm, Neurmedix, Orion Pharma, Otsuka, Pfizer, Pharma2B, Prana Biotechnology, Prothena, Neotope, Elan Pharmaceutical, Raptor Pharmaceuticals, Remedy Pharmaceuticals, Hoffmann-La Roche, Sage Bionetworks, Sanofi, Serina, Sunovion, Synagile, Titan, Upsher-Smith, US WorldMeds, Vaccinex, Vertex Pharmaceuticals, Weston Brain Institute. KK has also received grants or research support from National Institutes of Health National Institute of Neurological Disorders and Stroke, Michael J Fox Foundation, and Teva Pharmaceuticals. GBL has provided consulting services, advisory board functions, clinical trial services, or lectures for Alnylam, Amarin, AOP Orphan Pharmaceuticals, Bayer Pharma, Desitin, GlaxoSmithKline, Hoffmann-La Roche, Ipsen, Ionis Pharmaceuticals, Lundbeck, Neurosearch, Medesis, Medivation, Medtronic, Novartis, Pfizer, Prana Biotechnology, PTC Therapeutics, Raptor Pharmaceuticals, Sangamo and Shire, Siena Biotech, Temmler Pharma, Teva Pharmaceuticals, UniQure, and Wave Life Sciences and has received grants from CHDI, BMBF, DFG, and EU-FP7. His study site, University of Ulm, has received compensation in the context of the observational REGISTRY-Study of EHDN and the observational Enroll-HD study from CHDI, as well as from Teva Pharmaceuticals. DL declares no competing interests. We acknowledge the help and enthusiasm of the participants and caregivers and the investigators and staff at the participating sites; the support received from EHDN and HSG; the efforts of the DSMB under the leadership of Roger Albin; and Kathleen Blatt (former employee of Teva Pharmaceuticals), Helena Knebel (employee of Teva Pharmaceuticals), Gina Pastino (employee of Teva Pharmaceuticals), Leehee Navon-Perry (employee of Teva Pharmaceuticals), and Matthew D Davis (employee of Teva Pharmaceuticals) for their contributions to the study. Medical writing assistance (collation of comments, preparation of data tables, and final styling) was provided by Anita Chadha-Patel of ACP Clinical Communications and funded by Teva Branded Pharmaceutical Products R & D (Frazer, PA). This study was funded by Teva Pharmaceuticals.

Financiadores	Número del financiador
Deutsches Zentrum für Neurodegeneration und Entzündung
Siena Biotech
Temmler Pharma
Teva Branded Pharmaceutical Products R & D
uniQure
National Science Foundation
National Institute of Neurological Disorders and Stroke
Michael J. Fox Foundation for Parkinson's Research
CHDI Foundation
Teva Pharmaceutical Industries
F. Hoffmann-La Roche
Ionis Pharmaceuticals
European Huntington's Disease Network
Deutsche Forschungsgemeinschaft
Bundesministerium für Bildung und Forschung
Shire
Seventh Framework Programme
H. Lundbeck A/S
Ipsen

ASJC Scopus Subject Areas

Clinical Neurology

ODS de las Naciones Unidas

Este resultado contribuye a los siguientes Objetivos de Desarrollo Sostenible

Acceder al documento

10.1016/S1474-4422(18)30391-0

Otros archivos y enlaces

Citar esto

@article{4f8952bdef8145a38e593ed62ae1408b,

title = "Safety and efficacy of pridopidine in patients with Huntington's disease (PRIDE-HD): a phase 2, randomised, placebo-controlled, multicentre, dose-ranging study",

abstract = "Background: Previous trials have shown that pridopidine might reduce motor impairment in patients with Huntington's disease. The aim of this study was to ascertain whether higher doses of pridopidine than previously tested reduce motor symptoms in a dose-dependent manner while maintaining acceptable safety and tolerability. Methods: PRIDE-HD was a randomised, placebo-controlled, phase 2, dose-ranging study in adults (aged ≥21 years) with Huntington's disease at outpatient clinics in 53 sites across 12 countries (Australia, Austria, Canada, Denmark, France, Germany, Italy, Poland, Russia, the Netherlands, the UK, and the USA). Eligible patients had clinical onset after age 18 years, 36 or more cytosine-adenine-guanine repeats in the huntingtin gene, motor symptoms (Unified Huntington's Disease Rating Scale total motor score [UHDRS-TMS] ≥25 points), and reduced independence (UHDRS independence score ≤90%). Patients were randomly assigned (1:1:1:1:1) with centralised interactive-response technology to receive one of four doses of pridopidine (45, 67·5, 90, or 112·5 mg) or placebo orally twice a day for 52 weeks. Randomisation was stratified within centres by neuroleptic drug use. The primary efficacy endpoint was change in the UHDRS-TMS from baseline to 26 weeks, which was assessed in all randomised patients who received at least one dose of study drug and had at least one post-baseline efficacy assessment (full analysis set). Participants and investigators were masked to treatment assignment. This trial is registered with EudraCT (2013-001888-23) and ClinicalTrials.gov (NCT02006472). Findings: Between Feb 13, 2014, and July 5, 2016, 408 patients were enrolled and randomly assigned to receive placebo (n=82) or pridopidine 45 mg (n=81), 67·5 mg (n=82), 90 mg (n=81), or 112·5 mg (n=82) twice daily for 26 weeks. The full analysis set included 397 patients (81 in the placebo group, 75 in the 45 mg group, 79 in the 67·5 mg group, 81 in the 90 mg group, and 81 in the 112·5 mg group). Pridopidine did not significantly change the UHDRS-TMS at 26 weeks compared with placebo at any dose. The most frequent adverse events across all groups were diarrhoea, vomiting, nasopharyngitis, falls, headache, insomnia, and anxiety. The most common treatment-related adverse events were insomnia, diarrhoea, nausea, and dizziness. Serious adverse events occurred in the pridopidine groups only and were most frequently falls (n=5), suicide attempt (n=4), suicidal ideation (n=3), head injury (n=3), and aspiration pneumonia (n=3). No new safety or tolerability concerns emerged in this study. One death in the pridopidine 112·5 mg group due to aspiration pneumonia was considered to be possibly related to the study drug. Interpretation: Pridopidine did not improve the UHDRS-TMS at week 26 compared with placebo and, thus, the results of secondary or tertiary analyses in previous trials were not replicated. A potentially strong placebo effect needs to be ruled out in future studies. Funding: Teva Pharmaceutical Industries.",

author = "{European Huntington's Disease Network} and {Huntington Study Group investigators} and Ralf Reilmann and Andrew McGarry and Grachev, {Igor D.} and Savola, {Juha Matti} and Beth Borowsky and Eli Eyal and Nicholas Gross and Douglas Langbehn and Robin Schubert and Wickenberg, {Anna Teige} and Spyros Papapetropoulos and Michael Hayden and Ferdinando Squitieri and Karl Kieburtz and Landwehrmeyer, {G. Bernhard} and Pinky Agarwal and Anderson, {Karen E.} and Aziz, {Nasir A.} and Azulay, {Jean Phillippe} and Bachoud-Levi, {Anne C.} and Roger Barker and Agnieszka Bebak and Markus Beuth and Kevin Biglan and Stephanie Blin and Stefan Bohlen and Raphael Bonelli and Sue Caldwell and Fabienne Calvas and Jonielyn Carlos and Simona Castagliuolo and Terrence Chong and Phyllis Chua and Allison Coleman and Jody Corey-Bloom and Rebecca Cousins and David Craufurd and Jill Davison and Eric Decorte and {De Michele}, Giuseppe and Laura Dornhege and Andrew Feigin and Stephanie Gallehawk and Pascale Gauteul and Carey Gonzales and Jane Griffith and Alexander Gustov and Mark Guttman and Beatrix Heim and Karen Marder",

note = "Publisher Copyright: {\textcopyright} 2019 Elsevier Ltd",

year = "2019",

month = feb,

doi = "10.1016/S1474-4422(18)30391-0",

language = "English",

volume = "18",

pages = "165--176",

journal = "The Lancet Neurology",

issn = "1474-4422",

publisher = "Lancet Publishing Group",

number = "2",

}

TY - JOUR

T1 - Safety and efficacy of pridopidine in patients with Huntington's disease (PRIDE-HD)

T2 - a phase 2, randomised, placebo-controlled, multicentre, dose-ranging study

AU - European Huntington's Disease Network

AU - Huntington Study Group investigators

AU - Reilmann, Ralf

AU - McGarry, Andrew

AU - Grachev, Igor D.

AU - Savola, Juha Matti

AU - Borowsky, Beth

AU - Eyal, Eli

AU - Gross, Nicholas

AU - Langbehn, Douglas

AU - Schubert, Robin

AU - Wickenberg, Anna Teige

AU - Papapetropoulos, Spyros

AU - Hayden, Michael

AU - Squitieri, Ferdinando

AU - Kieburtz, Karl

AU - Landwehrmeyer, G. Bernhard

AU - Agarwal, Pinky

AU - Anderson, Karen E.

AU - Aziz, Nasir A.

AU - Azulay, Jean Phillippe

AU - Bachoud-Levi, Anne C.

AU - Barker, Roger

AU - Bebak, Agnieszka

AU - Beuth, Markus

AU - Biglan, Kevin

AU - Blin, Stephanie

AU - Bohlen, Stefan

AU - Bonelli, Raphael

AU - Caldwell, Sue

AU - Calvas, Fabienne

AU - Carlos, Jonielyn

AU - Castagliuolo, Simona

AU - Chong, Terrence

AU - Chua, Phyllis

AU - Coleman, Allison

AU - Corey-Bloom, Jody

AU - Cousins, Rebecca

AU - Craufurd, David

AU - Davison, Jill

AU - Decorte, Eric

AU - De Michele, Giuseppe

AU - Dornhege, Laura

AU - Feigin, Andrew

AU - Gallehawk, Stephanie

AU - Gauteul, Pascale

AU - Gonzales, Carey

AU - Griffith, Jane

AU - Gustov, Alexander

AU - Guttman, Mark

AU - Heim, Beatrix

AU - Marder, Karen

PY - 2019/2

Y1 - 2019/2

N2 - Background: Previous trials have shown that pridopidine might reduce motor impairment in patients with Huntington's disease. The aim of this study was to ascertain whether higher doses of pridopidine than previously tested reduce motor symptoms in a dose-dependent manner while maintaining acceptable safety and tolerability. Methods: PRIDE-HD was a randomised, placebo-controlled, phase 2, dose-ranging study in adults (aged ≥21 years) with Huntington's disease at outpatient clinics in 53 sites across 12 countries (Australia, Austria, Canada, Denmark, France, Germany, Italy, Poland, Russia, the Netherlands, the UK, and the USA). Eligible patients had clinical onset after age 18 years, 36 or more cytosine-adenine-guanine repeats in the huntingtin gene, motor symptoms (Unified Huntington's Disease Rating Scale total motor score [UHDRS-TMS] ≥25 points), and reduced independence (UHDRS independence score ≤90%). Patients were randomly assigned (1:1:1:1:1) with centralised interactive-response technology to receive one of four doses of pridopidine (45, 67·5, 90, or 112·5 mg) or placebo orally twice a day for 52 weeks. Randomisation was stratified within centres by neuroleptic drug use. The primary efficacy endpoint was change in the UHDRS-TMS from baseline to 26 weeks, which was assessed in all randomised patients who received at least one dose of study drug and had at least one post-baseline efficacy assessment (full analysis set). Participants and investigators were masked to treatment assignment. This trial is registered with EudraCT (2013-001888-23) and ClinicalTrials.gov (NCT02006472). Findings: Between Feb 13, 2014, and July 5, 2016, 408 patients were enrolled and randomly assigned to receive placebo (n=82) or pridopidine 45 mg (n=81), 67·5 mg (n=82), 90 mg (n=81), or 112·5 mg (n=82) twice daily for 26 weeks. The full analysis set included 397 patients (81 in the placebo group, 75 in the 45 mg group, 79 in the 67·5 mg group, 81 in the 90 mg group, and 81 in the 112·5 mg group). Pridopidine did not significantly change the UHDRS-TMS at 26 weeks compared with placebo at any dose. The most frequent adverse events across all groups were diarrhoea, vomiting, nasopharyngitis, falls, headache, insomnia, and anxiety. The most common treatment-related adverse events were insomnia, diarrhoea, nausea, and dizziness. Serious adverse events occurred in the pridopidine groups only and were most frequently falls (n=5), suicide attempt (n=4), suicidal ideation (n=3), head injury (n=3), and aspiration pneumonia (n=3). No new safety or tolerability concerns emerged in this study. One death in the pridopidine 112·5 mg group due to aspiration pneumonia was considered to be possibly related to the study drug. Interpretation: Pridopidine did not improve the UHDRS-TMS at week 26 compared with placebo and, thus, the results of secondary or tertiary analyses in previous trials were not replicated. A potentially strong placebo effect needs to be ruled out in future studies. Funding: Teva Pharmaceutical Industries.

AB - Background: Previous trials have shown that pridopidine might reduce motor impairment in patients with Huntington's disease. The aim of this study was to ascertain whether higher doses of pridopidine than previously tested reduce motor symptoms in a dose-dependent manner while maintaining acceptable safety and tolerability. Methods: PRIDE-HD was a randomised, placebo-controlled, phase 2, dose-ranging study in adults (aged ≥21 years) with Huntington's disease at outpatient clinics in 53 sites across 12 countries (Australia, Austria, Canada, Denmark, France, Germany, Italy, Poland, Russia, the Netherlands, the UK, and the USA). Eligible patients had clinical onset after age 18 years, 36 or more cytosine-adenine-guanine repeats in the huntingtin gene, motor symptoms (Unified Huntington's Disease Rating Scale total motor score [UHDRS-TMS] ≥25 points), and reduced independence (UHDRS independence score ≤90%). Patients were randomly assigned (1:1:1:1:1) with centralised interactive-response technology to receive one of four doses of pridopidine (45, 67·5, 90, or 112·5 mg) or placebo orally twice a day for 52 weeks. Randomisation was stratified within centres by neuroleptic drug use. The primary efficacy endpoint was change in the UHDRS-TMS from baseline to 26 weeks, which was assessed in all randomised patients who received at least one dose of study drug and had at least one post-baseline efficacy assessment (full analysis set). Participants and investigators were masked to treatment assignment. This trial is registered with EudraCT (2013-001888-23) and ClinicalTrials.gov (NCT02006472). Findings: Between Feb 13, 2014, and July 5, 2016, 408 patients were enrolled and randomly assigned to receive placebo (n=82) or pridopidine 45 mg (n=81), 67·5 mg (n=82), 90 mg (n=81), or 112·5 mg (n=82) twice daily for 26 weeks. The full analysis set included 397 patients (81 in the placebo group, 75 in the 45 mg group, 79 in the 67·5 mg group, 81 in the 90 mg group, and 81 in the 112·5 mg group). Pridopidine did not significantly change the UHDRS-TMS at 26 weeks compared with placebo at any dose. The most frequent adverse events across all groups were diarrhoea, vomiting, nasopharyngitis, falls, headache, insomnia, and anxiety. The most common treatment-related adverse events were insomnia, diarrhoea, nausea, and dizziness. Serious adverse events occurred in the pridopidine groups only and were most frequently falls (n=5), suicide attempt (n=4), suicidal ideation (n=3), head injury (n=3), and aspiration pneumonia (n=3). No new safety or tolerability concerns emerged in this study. One death in the pridopidine 112·5 mg group due to aspiration pneumonia was considered to be possibly related to the study drug. Interpretation: Pridopidine did not improve the UHDRS-TMS at week 26 compared with placebo and, thus, the results of secondary or tertiary analyses in previous trials were not replicated. A potentially strong placebo effect needs to be ruled out in future studies. Funding: Teva Pharmaceutical Industries.

UR - http://www.scopus.com/inward/record.url?scp=85060007351&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85060007351&partnerID=8YFLogxK

U2 - 10.1016/S1474-4422(18)30391-0

DO - 10.1016/S1474-4422(18)30391-0

M3 - Article

C2 - 30563778

AN - SCOPUS:85060007351

SN - 1474-4422

VL - 18

SP - 165

EP - 176

JO - The Lancet Neurology

JF - The Lancet Neurology

IS - 2

ER -

Safety and efficacy of pridopidine in patients with Huntington's disease (PRIDE-HD): a phase 2, randomised, placebo-controlled, multicentre, dose-ranging study

Resumen

Financiación

ASJC Scopus Subject Areas

ODS de las Naciones Unidas

Acceder al documento

Otros archivos y enlaces

Huella

Citar esto