Abstract
BACKGROUND: Apamin-sensitive small conductance calcium-activated K current (I(KAS)) is up-regulated during ventricular pacing and masks short-term cardiac memory (CM). OBJECTIVE: The purpose of this study was to determine the role of I(KAS) in long-term CM. METHODS: CM was created with 3-5 weeks of ventricular pacing and defined by a flat or inverted T wave off pacing. Epicardial optical mapping was performed in both paced and normal ventricles. Action potential duration (APD(80)) was determined during right atrial pacing. Ventricular stability was tested before and after I(KAS) blockade. Four paced hearts and 4 normal hearts were used for western blotting and histology. RESULTS: There were no significant differences in either echocardiographic parameters or fibrosis levels between groups. Apamin induced more APD(80) prolongation in CM than in normal ventricles (mean [95% confidence interval]: 9.6% [8.8%-10.5%] vs 3.1% [1.9%-4.3%]; P <.001). Apamin significantly lengthened APD(80) in the CM model at late activation sites, indicating significant I(KAS) up-regulation at those sites. The CM model also had altered Ca(2+) handling, with the 50% Ca(2+) transient duration and amplitude increased at distal sites compared to a proximal site (near the pacing site). After apamin, the CM model had increased ventricular fibrillation (VF) inducibility (paced vs control: 33/40 (82.5%) vs 7/20 (35%); P <.001) and longer VF durations (124 vs 26 seconds; P <.001). CONCLUSION: Chronic ventricular pacing increases Ca(2+) transients at late activation sites, which activates I(KAS) to maintain repolarization reserve. I(KAS) blockade increases VF vulnerability in chronically paced rabbit ventricles.