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Status: Bibliographieeintrag

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Verfasst von:Staudacher, Ingo [VerfasserIn]   i
 Schweizer, Patrick Alexander [VerfasserIn]   i
 Katus, Hugo [VerfasserIn]   i
 Thomas, Dierk [VerfasserIn]   i
Titel:hERG
Titelzusatz:protein trafficking and potential for therapy and drug side effects
Verf.angabe:Ingo Staudacher, Patrick A. Schweizer, Hugo A. Katus, Dierk Thomas
E-Jahr:2010
Jahr:2010 Jan
Umfang:8 S.
Fussnoten:Gesehen am 20.10.2023
Titel Quelle:Enthalten in: Current opinion in drug discovery & development
Ort Quelle:London : Thomson Scientific, 1998
Jahr Quelle:2010
Band/Heft Quelle:13(2010), 1, Seite 23-30
ISSN Quelle:1367-6733
Abstract:Drug-induced QT interval prolongation is associated with torsade de pointes arrhythmia and sudden cardiac death. Acquired long QT syndrome poses a significant liability in pharmaceutical drug development, and has resulted in drugs being recalled from the market. This off-target property is caused primarily by the inhibition of cardiac hERG K+ currents. As a result, guidelines were established by The International Conference on Harmonisation of Technical Requirements for Registration of Pharmaceuticals for Human Use (ICH) requiring the preclinical evaluation of direct hERG channel blockade and QT prolongation. This review discusses established, as well as newly discovered and currently under-recognized, pro-arrhythmic mechanisms that are associated with hERG protein trafficking. Defective hERG trafficking is a research area of intensive scientific activity, and the implementation of screening for this type of hERG liability should be considered in order to improve the risk assessment and detection of drug-associated cardiotoxicity in safety pharmacology.
Datenträger:Online-Ressource
Sprache:eng
Sach-SW:Animals
 Anti-Arrhythmia Agents
 Apoptosis
 ERG1 Potassium Channel
 Ether-A-Go-Go Potassium Channels
 Humans
 Long QT Syndrome
 Models, Molecular
 Protein Transport
 Torsades de Pointes
K10plus-PPN:1866744852
Verknüpfungen:→ Zeitschrift

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