Evidence for the hERG Liability of antihistamines, antipsychotics, and anti-infective agents: A systematic literature review from the ARITMO project
Evidence for the hERG Liability of antihistamines, antipsychotics, and anti-infective agents: A systematic literature review from the ARITMO project
A systematic review was performed to categorize the hERG (human ether-a-go-go–related gene) liability of antihistamines, antipsychotics, and anti-infectives and to compare it with current clinical risk of torsade de pointes (TdP). Eligible studies were hERG assays reporting half-minimal inhibitory concentrations (IC50). A “hERG safety margin” was calculated from the IC50 divided by the peak human plasma concentration (free Cmax). A margin below 30 defined hERG liability. Each drug was assigned an “uncertainty score” based on volume, consistency, precision, and internal and external validity of evidence. The hERG liability was compared to existing knowledge on TdP risk (www.credibledrugs.org). Of 1828 studies, 82 were eligible, allowing calculation of safety margins for 61 drugs. Thirty-one drugs (51%) had evidence of hERG liability including 6 with no previous mention of TdP risk (eg, desloratadine, lopinavir). Conversely, 16 drugs (26%) had no evidence of hERG liability including 6 with known, or at least conditional or possible, TdP risk (eg, chlorpromazine, sulpiride). The main sources of uncertainty were the validity of the experimental conditions used (antihistamines and antipsychotics) and nonuse of reference compounds (anti-infectives). In summary, hERG liability was categorized for 3 widely used drug classes, incorporating a qualitative assessment of the strength of available evidence. Some concordance with TdP risk was observed, although several drugs had hERG liability without evidence of clinical risk and vice versa. This may be due to gaps in clinical evidence, limitations of hERG/Cmax data, or other patient/drug-specific factors that contribute to real-life TdP risk.
anti-infective agents, antipsychotic agents, ether-a-go-go potassium channels, histamine H1 antagonists, review
558-572
Hazell, Lorna
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Raschi, Emanuel
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De Ponti, Fabrizio
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Thomas, Simon H.L.
bee904fe-3119-4495-859d-593a80153ee8
Salvo, Francesco
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Ahlberg Helgee, Ernst
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Boyer, Scott
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Sturkenboom, Miriam
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Shakir, Saad
648f9207-b801-4dc9-9f7f-b694bb4dc518
1 May 2017
Hazell, Lorna
1c9036d8-13c0-4fe1-88be-9a926dc003b5
Raschi, Emanuel
d851b687-ff98-4e41-8228-037048e63168
De Ponti, Fabrizio
dac23128-6eed-4897-ab96-7d0c5432d0e7
Thomas, Simon H.L.
bee904fe-3119-4495-859d-593a80153ee8
Salvo, Francesco
2e7651c7-4c18-4dc2-9a95-923bb32d2507
Ahlberg Helgee, Ernst
6c285e3a-dc33-493a-b285-a604b61ec2b8
Boyer, Scott
87f4275c-9a68-4b7e-9af3-ad54f7464270
Sturkenboom, Miriam
215880a2-31f9-47e1-8377-6d3fb122f5da
Shakir, Saad
648f9207-b801-4dc9-9f7f-b694bb4dc518
Hazell, Lorna, Raschi, Emanuel, De Ponti, Fabrizio, Thomas, Simon H.L., Salvo, Francesco, Ahlberg Helgee, Ernst, Boyer, Scott, Sturkenboom, Miriam and Shakir, Saad
(2017)
Evidence for the hERG Liability of antihistamines, antipsychotics, and anti-infective agents: A systematic literature review from the ARITMO project.
Journal of Clinical Pharmacology, 57 (5), .
(doi:10.1002/jcph.838).
Abstract
A systematic review was performed to categorize the hERG (human ether-a-go-go–related gene) liability of antihistamines, antipsychotics, and anti-infectives and to compare it with current clinical risk of torsade de pointes (TdP). Eligible studies were hERG assays reporting half-minimal inhibitory concentrations (IC50). A “hERG safety margin” was calculated from the IC50 divided by the peak human plasma concentration (free Cmax). A margin below 30 defined hERG liability. Each drug was assigned an “uncertainty score” based on volume, consistency, precision, and internal and external validity of evidence. The hERG liability was compared to existing knowledge on TdP risk (www.credibledrugs.org). Of 1828 studies, 82 were eligible, allowing calculation of safety margins for 61 drugs. Thirty-one drugs (51%) had evidence of hERG liability including 6 with no previous mention of TdP risk (eg, desloratadine, lopinavir). Conversely, 16 drugs (26%) had no evidence of hERG liability including 6 with known, or at least conditional or possible, TdP risk (eg, chlorpromazine, sulpiride). The main sources of uncertainty were the validity of the experimental conditions used (antihistamines and antipsychotics) and nonuse of reference compounds (anti-infectives). In summary, hERG liability was categorized for 3 widely used drug classes, incorporating a qualitative assessment of the strength of available evidence. Some concordance with TdP risk was observed, although several drugs had hERG liability without evidence of clinical risk and vice versa. This may be due to gaps in clinical evidence, limitations of hERG/Cmax data, or other patient/drug-specific factors that contribute to real-life TdP risk.
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Accepted/In Press date: 8 October 2016
e-pub ahead of print date: 26 December 2016
Published date: 1 May 2017
Keywords:
anti-infective agents, antipsychotic agents, ether-a-go-go potassium channels, histamine H1 antagonists, review
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Local EPrints ID: 439198
URI: http://eprints.soton.ac.uk/id/eprint/439198
ISSN: 0091-2700
PURE UUID: 57cdb570-f1dd-46f9-ad83-9ff4c885b89e
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Date deposited: 06 Apr 2020 16:36
Last modified: 10 May 2024 16:59
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Contributors
Author:
Emanuel Raschi
Author:
Fabrizio De Ponti
Author:
Simon H.L. Thomas
Author:
Francesco Salvo
Author:
Ernst Ahlberg Helgee
Author:
Scott Boyer
Author:
Miriam Sturkenboom
Author:
Saad Shakir
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