Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context

Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context

Background: The POP Trial was a phase 1, open-label, rising-dose, randomised study that explored the safety and tolerability of calmangafodipir (superoxide dismutase mimetic) co-treatment with n-acetylcysteine (NAC) for paracetamol overdose. Methods: Patients were recruited at the Royal Infirmary of...

Full description

Bibliographic Details
Main Authors: Emma E. Morrison, Katherine Oatey, Bernadette Gallagher, Julia Grahamslaw, Rachel O'Brien, Polly Black, Wilna Oosthuyzen, Robert J. Lee, Christopher J. Weir, Dennis Henriksen, James W. Dear
Format: Article
Language:English
Published: Elsevier 2019-08-01
Series:EBioMedicine
Online Access:http://www.sciencedirect.com/science/article/pii/S2352396419304487
id doaj-8634f94b06b647bf93d8be5200422d32
record_format Article
spelling doaj-8634f94b06b647bf93d8be5200422d322020-11-25T02:33:14ZengElsevierEBioMedicine2352-39642019-08-0146423430Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in contextEmma E. Morrison0Katherine Oatey1Bernadette Gallagher2Julia Grahamslaw3Rachel O'Brien4Polly Black5Wilna Oosthuyzen6Robert J. Lee7Christopher J. Weir8Dennis Henriksen9James W. Dear10Pharmacology, Therapeutics and Toxicology Unit, Centre for Cardiovascular Science, University of Edinburgh, UKEdinburgh Clinical Trials Unit, UKEmergency Medicine Research Group, Royal Infirmary of Edinburgh, UKEmergency Medicine Research Group, Royal Infirmary of Edinburgh, UKEmergency Medicine Research Group, Royal Infirmary of Edinburgh, UKEmergency Medicine Research Group, Royal Infirmary of Edinburgh, UKPharmacology, Therapeutics and Toxicology Unit, Centre for Cardiovascular Science, University of Edinburgh, UKEdinburgh Clinical Trials Unit, UKEdinburgh Clinical Trials Unit, UKPledPharma AB, Stockholm, SwedenPharmacology, Therapeutics and Toxicology Unit, Centre for Cardiovascular Science, University of Edinburgh, UK; Corresponding author.Background: The POP Trial was a phase 1, open-label, rising-dose, randomised study that explored the safety and tolerability of calmangafodipir (superoxide dismutase mimetic) co-treatment with n-acetylcysteine (NAC) for paracetamol overdose. Methods: Patients were recruited at the Royal Infirmary of Edinburgh (8th June 2017-10th May 2018). Inclusion criterion: adults within 24 h of a paracetamol overdose that required NAC. Within each of 3 sequential cohorts, participants were randomly assigned, with concealed allocation, to NAC and a single intravenous calmangafodipir dose (n = 6) or NAC alone (n = 2). Calmangafodipir doses were 2, 5, or 10 μmol/kg. Participants, study and clinical teams were not blinded. The primary outcome was safety and tolerability. Secondary outcomes were alanine transaminase (ALT), international normalised ratio (INR), keratin-18, caspase-cleaved keratin-18 (ccK18), microRNA-122, and glutamate dehydrogenase (GLDH). (Clinicaltrials.gov:NCT03177395). Findings: All 24 participants received their allocated drug doses and were analysed. Primary endpoints: all participants experienced ≥1 adverse event (AE), most commonly gastrointestinal. Patients experiencing ≥1 serious adverse event (SAE): NAC alone, 2/6; NAC + calmangafodipir (2 μmol/kg), 4/6; NAC + calmangafodipir (5 μmol/kg), 2/6; NAC + calmangafodipir (10 μmol/kg), 3/6. No AEs or SAEs were probably or definitely calmangafodipir-related. Secondary safety outcomes demonstrated no differences between groups. With NAC alone, 2/6 had ALT > 100 U/L; with NAC + calmangafodipir, 0/18. No INR difference. Keratin-18 and ccK18 increased in the NAC alone group more than with calmangafodipir (baseline to 20 h fold change, NAC + calmangafodipir (5 μmol/kg) compared to NAC alone: 0.48 (95%CI 0.28–0.83)). microRNA-122 changes were similar to K18, GLDH was frequently undetected. Interpretation: Calmangafodipir was tolerated when combined with NAC and may reduce biomarkers of paracetamol toxicity.http://www.sciencedirect.com/science/article/pii/S2352396419304487
collection DOAJ
language English
format Article
sources DOAJ
author Emma E. Morrison
Katherine Oatey
Bernadette Gallagher
Julia Grahamslaw
Rachel O'Brien
Polly Black
Wilna Oosthuyzen
Robert J. Lee
Christopher J. Weir
Dennis Henriksen
James W. Dear
spellingShingle Emma E. Morrison
Katherine Oatey
Bernadette Gallagher
Julia Grahamslaw
Rachel O'Brien
Polly Black
Wilna Oosthuyzen
Robert J. Lee
Christopher J. Weir
Dennis Henriksen
James W. Dear
Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context
EBioMedicine
author_facet Emma E. Morrison
Katherine Oatey
Bernadette Gallagher
Julia Grahamslaw
Rachel O'Brien
Polly Black
Wilna Oosthuyzen
Robert J. Lee
Christopher J. Weir
Dennis Henriksen
James W. Dear
author_sort Emma E. Morrison
title Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context
title_short Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context
title_full Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context
title_fullStr Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context
title_full_unstemmed Principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of N-acetylcysteine for paracetamol overdose (POP trial)Research in context
title_sort principal results of a randomised open label exploratory, safety and tolerability study with calmangafodipir in patients treated with a 12 h regimen of n-acetylcysteine for paracetamol overdose (pop trial)research in context
publisher Elsevier
series EBioMedicine
issn 2352-3964
publishDate 2019-08-01
description Background: The POP Trial was a phase 1, open-label, rising-dose, randomised study that explored the safety and tolerability of calmangafodipir (superoxide dismutase mimetic) co-treatment with n-acetylcysteine (NAC) for paracetamol overdose. Methods: Patients were recruited at the Royal Infirmary of Edinburgh (8th June 2017-10th May 2018). Inclusion criterion: adults within 24 h of a paracetamol overdose that required NAC. Within each of 3 sequential cohorts, participants were randomly assigned, with concealed allocation, to NAC and a single intravenous calmangafodipir dose (n = 6) or NAC alone (n = 2). Calmangafodipir doses were 2, 5, or 10 μmol/kg. Participants, study and clinical teams were not blinded. The primary outcome was safety and tolerability. Secondary outcomes were alanine transaminase (ALT), international normalised ratio (INR), keratin-18, caspase-cleaved keratin-18 (ccK18), microRNA-122, and glutamate dehydrogenase (GLDH). (Clinicaltrials.gov:NCT03177395). Findings: All 24 participants received their allocated drug doses and were analysed. Primary endpoints: all participants experienced ≥1 adverse event (AE), most commonly gastrointestinal. Patients experiencing ≥1 serious adverse event (SAE): NAC alone, 2/6; NAC + calmangafodipir (2 μmol/kg), 4/6; NAC + calmangafodipir (5 μmol/kg), 2/6; NAC + calmangafodipir (10 μmol/kg), 3/6. No AEs or SAEs were probably or definitely calmangafodipir-related. Secondary safety outcomes demonstrated no differences between groups. With NAC alone, 2/6 had ALT > 100 U/L; with NAC + calmangafodipir, 0/18. No INR difference. Keratin-18 and ccK18 increased in the NAC alone group more than with calmangafodipir (baseline to 20 h fold change, NAC + calmangafodipir (5 μmol/kg) compared to NAC alone: 0.48 (95%CI 0.28–0.83)). microRNA-122 changes were similar to K18, GLDH was frequently undetected. Interpretation: Calmangafodipir was tolerated when combined with NAC and may reduce biomarkers of paracetamol toxicity.
url http://www.sciencedirect.com/science/article/pii/S2352396419304487
work_keys_str_mv AT emmaemorrison principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT katherineoatey principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT bernadettegallagher principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT juliagrahamslaw principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT rachelobrien principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT pollyblack principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT wilnaoosthuyzen principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT robertjlee principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT christopherjweir principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT dennishenriksen principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
AT jameswdear principalresultsofarandomisedopenlabelexploratorysafetyandtolerabilitystudywithcalmangafodipirinpatientstreatedwitha12hregimenofnacetylcysteineforparacetamoloverdosepoptrialresearchincontext
_version_ 1724815480591482880

Similar Items