Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial

BACKGROUND: The propagation of prions, the causative agents of Creutzfeldt-Jakob disease and other human prion diseases, requires post-translational conversion of normal cellular prion protein to disease-associated forms. The antimalarial drug quinacrine (mepacrine) prevents this conversion in vitro...

Descripción completa

Detalles Bibliográficos
Autores principales: Collinge, John, Gorham, Michele, Hudson, Fleur, Kennedy, Angus, Keogh, Geraldine, Pal, Suvankar, Rossor, Martin, Rudge, Peter, Siddique, Durre, Spyer, Moira, Thomas, Dafydd, Walker, Sarah, Webb, Tom, Wroe, Steve, Darbyshire, Janet
Formato: Texto
Lenguaje:English
Publicado: Lancet Pub. Group 2009
Materias:
Fast track — Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2660392/
https://www.ncbi.nlm.nih.gov/pubmed/19278902
http://dx.doi.org/10.1016/S1474-4422(09)70049-3
_version_ 1782165726157602816
author Collinge, John
Gorham, Michele
Hudson, Fleur
Kennedy, Angus
Keogh, Geraldine
Pal, Suvankar
Rossor, Martin
Rudge, Peter
Siddique, Durre
Spyer, Moira
Thomas, Dafydd
Walker, Sarah
Webb, Tom
Wroe, Steve
Darbyshire, Janet
author_facet Collinge, John
Gorham, Michele
Hudson, Fleur
Kennedy, Angus
Keogh, Geraldine
Pal, Suvankar
Rossor, Martin
Rudge, Peter
Siddique, Durre
Spyer, Moira
Thomas, Dafydd
Walker, Sarah
Webb, Tom
Wroe, Steve
Darbyshire, Janet
author_sort Collinge, John
collection PubMed
description BACKGROUND: The propagation of prions, the causative agents of Creutzfeldt-Jakob disease and other human prion diseases, requires post-translational conversion of normal cellular prion protein to disease-associated forms. The antimalarial drug quinacrine (mepacrine) prevents this conversion in vitro, and was given to patients with various prion diseases to assess its safety and efficacy in changing the course of these invariably fatal and untreatable diseases. METHODS: Patients with prion disease were recruited via the UK national referral system and were offered a choice between quinacrine (300 mg daily), no quinacrine, or randomisation to immediate quinacrine or deferred quinacrine in an open-label, patient-preference trial. The primary endpoints were death and serious adverse events possibly or probably related to the study drug. This study is registered, ISRCTN 06722585. FINDINGS: 107 patients with prion disease (45 sporadic, two iatrogenic, 18 variant, and 42 inherited) were enrolled, 23 in a pilot study and 84 in the main study. Only two patients chose randomisation; 40 took quinacrine during follow-up (37 who chose it at enrolment). Choice of treatment was associated with disease severity, with those least and most severely affected more likely to choose not to receive quinacrine. 78 (73%) patients died: one randomly assigned to deferred treatment, 26 of 38 who chose immediate quinacrine, and 51 of 68 who chose no quinacrine. Although adjusted mortality was lower in those who chose to take quinacrine than in those who did not, this was due to confounding with disease severity, and there was no difference in mortality between groups after adjustment. Four of 40 patients who took quinacrine had a transient response on neurological rating scales. Only two of 14 reported serious adverse events were judged quinacrine-related. INTERPRETATION: Quinacrine at a dose of 300 mg per day was reasonably tolerated but did not significantly affect the clinical course of prion diseases in this observational study. FUNDING: Department of Health (England); UK Medical Research Council.
format Text
id pubmed-2660392
institution National Center for Biotechnology Information
language English
publishDate 2009
publisher Lancet Pub. Group
record_format MEDLINE/PubMed
spelling pubmed-26603922009-04-16 Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial Collinge, John Gorham, Michele Hudson, Fleur Kennedy, Angus Keogh, Geraldine Pal, Suvankar Rossor, Martin Rudge, Peter Siddique, Durre Spyer, Moira Thomas, Dafydd Walker, Sarah Webb, Tom Wroe, Steve Darbyshire, Janet Lancet Neurol Fast track — Articles BACKGROUND: The propagation of prions, the causative agents of Creutzfeldt-Jakob disease and other human prion diseases, requires post-translational conversion of normal cellular prion protein to disease-associated forms. The antimalarial drug quinacrine (mepacrine) prevents this conversion in vitro, and was given to patients with various prion diseases to assess its safety and efficacy in changing the course of these invariably fatal and untreatable diseases. METHODS: Patients with prion disease were recruited via the UK national referral system and were offered a choice between quinacrine (300 mg daily), no quinacrine, or randomisation to immediate quinacrine or deferred quinacrine in an open-label, patient-preference trial. The primary endpoints were death and serious adverse events possibly or probably related to the study drug. This study is registered, ISRCTN 06722585. FINDINGS: 107 patients with prion disease (45 sporadic, two iatrogenic, 18 variant, and 42 inherited) were enrolled, 23 in a pilot study and 84 in the main study. Only two patients chose randomisation; 40 took quinacrine during follow-up (37 who chose it at enrolment). Choice of treatment was associated with disease severity, with those least and most severely affected more likely to choose not to receive quinacrine. 78 (73%) patients died: one randomly assigned to deferred treatment, 26 of 38 who chose immediate quinacrine, and 51 of 68 who chose no quinacrine. Although adjusted mortality was lower in those who chose to take quinacrine than in those who did not, this was due to confounding with disease severity, and there was no difference in mortality between groups after adjustment. Four of 40 patients who took quinacrine had a transient response on neurological rating scales. Only two of 14 reported serious adverse events were judged quinacrine-related. INTERPRETATION: Quinacrine at a dose of 300 mg per day was reasonably tolerated but did not significantly affect the clinical course of prion diseases in this observational study. FUNDING: Department of Health (England); UK Medical Research Council. Lancet Pub. Group 2009-04 /pmc/articles/PMC2660392/ /pubmed/19278902 http://dx.doi.org/10.1016/S1474-4422(09)70049-3 Text en © 2009 Elsevier Ltd. All rights reserved. https://creativecommons.org/licenses/by/4.0/This work is licensed under a Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/) , which allows reusers to distribute, remix, adapt, and build upon the material in any medium or format, so long as attribution is given to the creator. The license allows for commercial use.
spellingShingle Fast track — Articles
Collinge, John
Gorham, Michele
Hudson, Fleur
Kennedy, Angus
Keogh, Geraldine
Pal, Suvankar
Rossor, Martin
Rudge, Peter
Siddique, Durre
Spyer, Moira
Thomas, Dafydd
Walker, Sarah
Webb, Tom
Wroe, Steve
Darbyshire, Janet
Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial
title Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial
title_full Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial
title_fullStr Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial
title_full_unstemmed Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial
title_short Safety and efficacy of quinacrine in human prion disease (PRION-1 study): a patient-preference trial
title_sort safety and efficacy of quinacrine in human prion disease (prion-1 study): a patient-preference trial
topic Fast track — Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2660392/
https://www.ncbi.nlm.nih.gov/pubmed/19278902
http://dx.doi.org/10.1016/S1474-4422(09)70049-3
work_keys_str_mv AT collingejohn safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT gorhammichele safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT hudsonfleur safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT kennedyangus safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT keoghgeraldine safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT palsuvankar safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT rossormartin safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT rudgepeter safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT siddiquedurre safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT spyermoira safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT thomasdafydd safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT walkersarah safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT webbtom safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT wroesteve safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial
AT darbyshirejanet safetyandefficacyofquinacrineinhumanpriondiseaseprion1studyapatientpreferencetrial

Ejemplares similares