Physiology of the Escape Rhythm After Radiofrequency Atrioventricular Junctional Ablation

• Published in: Pacing and clinical electrophysiology Vol. 21; no. 5; pp. 1085 - 1092
• Main Authors: SHEPARD, RICHARD K., NATALE, ANDREA, STAMBLER, BRUCE S., WOOD, MARK A., GILLIGAN, DAVID M., ELLENBOGEN, KENNETH A.
• Format: Journal Article
• Language: English
• Published: Oxford, UK Blackwell Publishing Ltd 01.05.1998
• Subjects: Adenosine - pharmacology; Aged; Anti-Arrhythmia Agents - pharmacology; atrial fibrillation; Atrial Fibrillation - surgery; Atrioventricular Node - physiology; Atrioventricular Node - surgery; Atropine - pharmacology; AV junction ablation; Bundle-Branch Block - etiology; Cardiac Pacing, Artificial; Cardiotonic Agents - pharmacology; Catheter Ablation; Female; Heart Rate - drug effects; Humans; Isoproterenol - pharmacology; Lidocaine - pharmacology; Male; radiofrequency ablation; Verapamil - pharmacology
• ISSN: 0147-8389; 1540-8159
• DOI: 10.1111/j.1540-8159.1998.tb00154.x

The physiology of the escape rhythm (ER) and its response to pharmacological modulation under varying autonomic conditions were studied in 48 patients undergoing radiofrequency ablation of the atrioventricular junction (AVJ) for refractory atrial fibrillation. The QRS morphology and cycle length (CL) of the baseline ER were measured 15 minutes postablation. The CL of the ER was measured in response to doses of isoproterenol, atropine, adenosine, lidocaine, and verapamil. The ER QRS was narrow (QRS < 120 ms) in 20 patients and wide (QRS > 120 ms) in 28 patients. Of the 28 patients with wide QRS ER, 11 patients had a new bundle branch block (8 patients new right bundle branch block [RBBB] and 2 patients new left bundle branch block [LBBB]). The ERCL was similar in both narrow and wide ERs (1,593 ± 376 ms and 1,516 ± 296 ms, P = 0.44). In 23 patients receiving isoproterenol infusion, the ER CL decreased with increasing doses from 1 mcg/min to 2 mcg/min (1,378 ± 200 to 1,240 ± 229 ms, P < 0.001), but did not decrease further at 3 mcg/min [1,201 ±192 ms, P = 0.48 vs 2 mg/min). Seven patients received 0.02 mg/kg of atropine, and ER decreased significantly (1,572 ± 408 ms to 1,319 ± 333 ms, P = 0.028). In 30 patients who received intravenous boluses of adenosine (6–18 mg), the ER did not change significantly. In 28 patients who received 150 mg of lidocaine, the ER increased from 1,462 ± 286 ms to 1,715 ± 467 ms (P < 0.001), and one patient developed transient asystole. Nineteen patients received 7.5 mg of verapamil, and the ER did not change (1,488 ± 313 ms to 1,513 ± 666 ms, P = 0.80). There was no significant difference in response to isoproterenol, adenosine, lidocaine, or verapamil between the patients with wide and narrow QRS ERs. We conclude that patients may have stable ERs immediately following AVJ ablation even when a wide complex ER results. The ER is responsive to sympathetic stimulation and vagal blockade. The ER is prolonged after lidocaine but not after verapamil, suggesting response to sodium but not to calcium channel blockade. These data are consistent with an ER originating in the distal compact AV node or proximal His bundle.