Inhibition of HERG potassium channels by cocaethylene: a metabolite of cocaine and ethanol

doi:10.1016/S0008-6363(01)00458-8

Cardiovascular Research 2002 53(1):59-67; doi:10.1016/S0008-6363(01)00458-8
© 2002 by European Society of Cardiology

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Inhibition of HERG potassium channels by cocaethylene: a metabolite of cocaine and ethanol

Michael E O'Leary^*

Department of Pathology, Anatomy and Cell Biology, Jefferson Medical College, 1020 Locust Street, Philadelphia, PA 19107, USA

michael.oleary{at}mail.tju.edu

^* Tel.: +1-215-503-9983; fax: +1-215-923-2218

Objective: To investigate the mechanism by which cocaethylene,a metabolite of cocaine and alcohol inhibits a cardiac delayedrectifier potassium channel. Methods: The cDNA of the HERG potassiumchannel that underlies I_Kr in humans was transiently expressedin tsA201 cells and currents recorded using the patch clamptechnique. Results: The cocaethylene inhibition of HERG is concentration-dependentwith an IC₅₀ of 4.0 µM. The inhibition increases overthe range of voltages where the channels activate suggestingthat cocaethylene binding may be linked to the activation oropening of the channels. Cocaethylene slows the deactivationof the tail current indicating that drug-modified channels arestabilized in the open conformation. Cocaethylene also acceleratesinactivation but has no effect of the recovery from inactivation.Conclusions: Cocaethylene inhibits HERG by binding to the activatedor open channels and by modulating the kinetics of inactivation.The cocaethylene inhibition of the channels occurs within therange of concentrations detected in the plasma of humans followingthe ingestion of cocaine and alcohol and is likely to contributeto the potent cardiotoxicity of this drug combination.

KEYWORDS Ion channels; K-channel; Long QT syndrome; Membrane currents

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