The contribution of national spontaneous reporting systems to detect signals of torsadogenicity: issues emerging from the ARITMO project
The contribution of national spontaneous reporting systems to detect signals of torsadogenicity: issues emerging from the ARITMO project
Introduction: Spontaneous reporting systems (SRSs) are pivotal for signal detection, especially for rare events with a high drug-attributable component, such as torsade de pointes (TdP). Use of different national SRSs is rarely attempted because of inherent difficulties, but should be considered on the assumption that rare events are diluted in international databases.
Objective: The aim was to describe TdP-related events associated with antipsychotics, H1-antihistamines and anti-infectives in three national SRSs (in Italy, Germany and France) and highlight potential signals of torsadogenicity through a combined literature evaluation.
Methods: A common search strategy was applied to extract TdP-related events: (1) TdP, (2) QT interval abnormalities, (3) ventricular fibrillation/tachycardia, and (4) sudden cardiac death. Signals of disproportionate reporting (SDRs) were calculated for TdP + QT interval abnormalities and defined by a lower limit of the 95 % confidence interval of the reporting odds ratio (ROR) >1. Among SDRs with at least three cases without concomitant pro-arrhythmic drugs, we defined potential new signal of torsadogenicity as drugs with no published evidence from (a) the crediblemeds® website (http://www.crediblemeds.com, as of November 1st, 2014); (b) studies on the FDA Adverse Event Reporting System (FAERS); and (c) safety trials or pharmaco-epidemiological studies (as of December 16th, 2014).
Results: Overall, 3505 cases were retrieved (1372, 1468, and 801 for France, Germany and Italy, respectively). Antipsychotics were mainly recorded in Germany (792 cases), whereas antibiotics peaked at 515 and 491 (France and Italy, respectively). Forty-one drugs met criteria for SDRs in at least one single source, of which 31 were detected only from one single SRS: 18, ten and three (French, German and Italian SRS, respectively). By contrast, only five SDRs were detected in all national data sources (amisulpride, aripiprazole, haloperidol, olanzapine, risperidone). Overall, five potential new signals of torsadogenicity were identified: flupentixol, ganciclovir, levocetirizine, oxatomide and tiapride.
Conclusions: We found differences across and within national SRSs in the reporting of drug-induced TdP, which finally resulted in five potential new signals of torsadogenicity. These findings warrant targeted pharmacovigilance studies to formally assess the existence of actual drug–event associations.
59-68
Raschi, Emanuel
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Poluzzi, Elisabetta
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Salvo, Francesco
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Koci, Ariola
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Suling, Marc
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Antoniazzi, Stefania
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Perina, Luisella
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Hazell, Lorna
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Moretti, Ugo
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Sturkenboom, Miriam
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Garbe, Edeltraut
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Pariente, Antoine
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De Ponti, Fabrizio
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1 January 2016
Raschi, Emanuel
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Poluzzi, Elisabetta
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Salvo, Francesco
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Koci, Ariola
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Suling, Marc
26571cfc-b53c-475b-adfc-3728f083d4c2
Antoniazzi, Stefania
19d0c38c-b3fd-4676-984f-f1d1ee61d84f
Perina, Luisella
dc10b758-ccba-4027-8f40-023e9663542b
Hazell, Lorna
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Moretti, Ugo
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Sturkenboom, Miriam
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Garbe, Edeltraut
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Pariente, Antoine
1bd75e3c-6938-4b44-9b25-067493573958
De Ponti, Fabrizio
dac23128-6eed-4897-ab96-7d0c5432d0e7
Raschi, Emanuel, Poluzzi, Elisabetta, Salvo, Francesco, Koci, Ariola, Suling, Marc, Antoniazzi, Stefania, Perina, Luisella, Hazell, Lorna, Moretti, Ugo, Sturkenboom, Miriam, Garbe, Edeltraut, Pariente, Antoine and De Ponti, Fabrizio
(2016)
The contribution of national spontaneous reporting systems to detect signals of torsadogenicity: issues emerging from the ARITMO project.
Drug Safety, 39 (1), .
(doi:10.1007/s40264-015-0353-1).
Abstract
Introduction: Spontaneous reporting systems (SRSs) are pivotal for signal detection, especially for rare events with a high drug-attributable component, such as torsade de pointes (TdP). Use of different national SRSs is rarely attempted because of inherent difficulties, but should be considered on the assumption that rare events are diluted in international databases.
Objective: The aim was to describe TdP-related events associated with antipsychotics, H1-antihistamines and anti-infectives in three national SRSs (in Italy, Germany and France) and highlight potential signals of torsadogenicity through a combined literature evaluation.
Methods: A common search strategy was applied to extract TdP-related events: (1) TdP, (2) QT interval abnormalities, (3) ventricular fibrillation/tachycardia, and (4) sudden cardiac death. Signals of disproportionate reporting (SDRs) were calculated for TdP + QT interval abnormalities and defined by a lower limit of the 95 % confidence interval of the reporting odds ratio (ROR) >1. Among SDRs with at least three cases without concomitant pro-arrhythmic drugs, we defined potential new signal of torsadogenicity as drugs with no published evidence from (a) the crediblemeds® website (http://www.crediblemeds.com, as of November 1st, 2014); (b) studies on the FDA Adverse Event Reporting System (FAERS); and (c) safety trials or pharmaco-epidemiological studies (as of December 16th, 2014).
Results: Overall, 3505 cases were retrieved (1372, 1468, and 801 for France, Germany and Italy, respectively). Antipsychotics were mainly recorded in Germany (792 cases), whereas antibiotics peaked at 515 and 491 (France and Italy, respectively). Forty-one drugs met criteria for SDRs in at least one single source, of which 31 were detected only from one single SRS: 18, ten and three (French, German and Italian SRS, respectively). By contrast, only five SDRs were detected in all national data sources (amisulpride, aripiprazole, haloperidol, olanzapine, risperidone). Overall, five potential new signals of torsadogenicity were identified: flupentixol, ganciclovir, levocetirizine, oxatomide and tiapride.
Conclusions: We found differences across and within national SRSs in the reporting of drug-induced TdP, which finally resulted in five potential new signals of torsadogenicity. These findings warrant targeted pharmacovigilance studies to formally assess the existence of actual drug–event associations.
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Raschi 2016 Article The Contribution Of National
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e-pub ahead of print date: 8 October 2015
Published date: 1 January 2016
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Local EPrints ID: 438869
URI: http://eprints.soton.ac.uk/id/eprint/438869
ISSN: 0114-5916
PURE UUID: d77af2a8-2315-47c7-816e-25a43d7e089f
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Date deposited: 25 Mar 2020 17:52
Last modified: 16 Mar 2024 06:53
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Author:
Emanuel Raschi
Author:
Elisabetta Poluzzi
Author:
Francesco Salvo
Author:
Ariola Koci
Author:
Marc Suling
Author:
Stefania Antoniazzi
Author:
Luisella Perina
Author:
Ugo Moretti
Author:
Miriam Sturkenboom
Author:
Edeltraut Garbe
Author:
Antoine Pariente
Author:
Fabrizio De Ponti
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