Chronic atrial ionic remodeling by aldosterone: potentiation of L-type Ca 2+ channels and its arrhythmogenic significance

It is widely accepted that aldosterone induces atrial fibrillation (AF) by promoting structural changes, but its effects on the function of primary atrial myocytes remain unknown. We have investigated this point in adult rat atrial myocytes, chronically exposed to the hormone. This treatment produce...

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Bibliographic Details
Published in:Pflügers Archiv 2016-11, Vol.468 (11-12), p.1823
Main Authors: Ríos-Pérez, Erick B, García-Castañeda, Maricela, Monsalvo-Villegas, Adrián, Avila, Guillermo
Format: Article
Language:English
Subjects:
Action Potentials - drug effects
Aldosterone - pharmacology
Animals
Calcium Channels, L-Type - metabolism
Cells, Cultured
Cyclic AMP - metabolism
Heart Atria - cytology
Heart Atria - metabolism
Male
Myocytes, Cardiac - drug effects
Myocytes, Cardiac - metabolism
Myocytes, Cardiac - physiology
Rats
Rats, Wistar
Receptors, Mineralocorticoid - metabolism
Sodium Channels - metabolism
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Summary:It is widely accepted that aldosterone induces atrial fibrillation (AF) by promoting structural changes, but its effects on the function of primary atrial myocytes remain unknown. We have investigated this point in adult rat atrial myocytes, chronically exposed to the hormone. This treatment produced larger amplitude of Ca transients, longer action potential (AP) duration, and higher incidence of unsynchronized Ca oscillations. Moreover, it also gave rise to increases in both cell membrane capacitance (C , 30 %) and activity of L-type Ca channels (LTCCs, 100 %). Concerning K currents, a twofold increase was also observed, but only in a delayed rectifier component (I ). Interestingly, the maximal conductance (G ) of Na channels was also enhanced, but it occurred in the face of a negative shift in the voltage dependence of inactivation. Thus, at physiological potentials, a decreased fraction of available channels neutralized the effect on G . With regard to the effects on both C and LTCCs, they involved activation of mineralocorticoid receptors (MRs), were dose-dependent (EC ∼20-130 nM), and developed and recovered in days. Neither gating currents nor protein levels of LTCCs were altered. Instead, the effect on LTCCs was mimicked by cAMP, reverted by a PKA inhibitor, and attenuated by a nitric oxide donor (short-term exposures). Both EGTA and the antioxidant NAC prevented the increase in C , without significantly interfering with the upregulation of LTCCs. Overall, these results show that chronic exposures to aldosterone result in dire functional changes at the single myocyte level, which may explain the link between aldosteronism and AF.
ISSN:1432-2013