Reverse rate dependency is an intrinsic property of canine cardiac preparations

doi:10.1093/cvr/cvp213

Cardiovascular Research Advance Access originally published online on June 25, 2009
Cardiovascular Research 2009 84(2):237-244; doi:10.1093/cvr/cvp213

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Reverse rate dependency is an intrinsic property of canine cardiac preparations

Tamás Bányász¹, Balázs Horváth¹, László Virág², László Bárándi¹, Norbert Szentandrássy¹, Gábor Harmati¹, János Magyar¹, Stefano Marangoni³, Antonio Zaza³, András Varró²^,4 and Péter P. Nánási¹^,*

¹ Department of Physiology, University of Debrecen, Nagyerdei krt 98, PO Box: 22, H-4012 Debrecen, Hungary
² Department of Pharmacology and Pharmacotherapy, University of Szeged, Szeged, Hungary
³ Dipartimento di Biotecnologie e Bioscienze, Universita di Milano-Bicocca, Milano, Italy
⁴ Division of Cardiovascular Pharmacology, Hungarian Academy of Sciences, Szeged, Hungary

^* Corresponding author. Tel: +36 52 416634; fax: +36 52 432289. E-mail address: nanasi{at}phys.dote.hu

Aims: Class III antiarrhythmic agents exhibit reverse rate-dependentlengthening of the action potential duration (APD). In spiteof the several theories developed so far to explain this reverserate dependency (RRD), its mechanism has not yet been clarified.The aim of the present work was to further elucidate the mechanismsresponsible for reverse rate-dependent drug effects.

Methods and results: Action potentials were recorded from multicellular canine ventricularpreparations and isolated cardiomyocytes, at cycle lengths (CLs)varying from 0.3 to 5 s, using conventional sharp microelectrodes.APD was either modified by applying inward and outward currentpulses, or by superfusion of agents known to lengthen and shortenAPD. Net membrane current (I_m) was calculated from action potentialwaveforms. The hypothesis that RRD may be implicit in the relationshipbetween I_m and APD was tested by numerical modelling. Both drug-inducedlengthening (by veratrine, BAY-K 8644, dofetilide, and BaCl₂)and shortening (by lidocaine and nicorandil) of action potentialsdisplayed RRD, i.e. changes in APD were greater at longer thanat shorter CL. A similar dependency of effect on CL was foundwhen repolarization was modified by injection of inward or outwardcurrent pulses. I_m measured at various points during repolarizationwas inversely proportional to APD and to CL. Model simulationsshowed that RRD is expected as a consequence of the non-linearityof the relationship between I_m and APD.

Conclusion: RRD of APD modulation is shared, although with differences inmagnitude, by interventions of very different nature. RRD canbe interpreted as a consequence of the relationship betweenI_m and APD and, as such, is expected in all species having positiveAPD–CL relationship. This implies that the developmentof agents prolonging APD with direct rate dependency, or evencompletely devoid of RRD, may be difficult to achieve.

KEYWORDS Action potential duration; Reverse rate dependence; Ventricular repolarization; Membrane current; Dog myocytes

Time for primary review: 22 days

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