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Circulation. 1998;97:369-380

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(Circulation. 1998;97:369-380.)
© 1998 American Heart Association, Inc.


Clinical Investigation and Reports

Body Surface Mapping During Pacing at Multiple Sites in the Human Atrium

P-Wave Morphology of Ectopic Right Atrial Activation

Arne SippensGroenewegen, MD; Heidi A. P. Peeters, MD; Emile R. Jessurun, MD; Andre C. Linnenbank, PhD; Etienne O. Robles de Medina, MD; Michael D. Lesh, MD; ; Norbert M. van Hemel, MD

From the Section of Cardiac Electrophysiology, Department of Medicine and the Cardiovascular Research Institute (A.S., M.D.L.), University of California at San Francisco; the Department of Cardiology (H.A.P.P., E.O.R.de M.), Heart Lung Institute, University Hospital and State University of Utrecht, the Netherlands; the Department of Cardiology (E.R.J., N.M.van H.), Antonius Hospital, Nieuwegein, the Netherlands; and the Laboratory of Medical Physics (A.C.L.), Academic Medical Center, University of Amsterdam, the Netherlands.

Correspondence to Arne SippensGroenewegen, MD, Section of Cardiac Electrophysiology, Department of Medicine, University of California at San Francisco, 500 Parnassus Ave, MU-East 4S, Box 1354, San Francisco, CA 94143-1354. E-mail sippens{at}ep4.ucsf.edu

Background—The morphology and polarity of the P wave on 12-lead ECG are of limited clinical value in localizing ectopic atrial rhythms. It was the aim of this study to assess the spatial resolution of body surface P-wave integral mapping in identifying the site of origin of ectopic right atrial (RA) impulse formation in patients without structural atrial disease.

Methods and Results—Sixty-two–lead ECG recordings were obtained during RA pacing at 86 distinct endocardial sites in nine patients with normal biatrial anatomy. After P-wave integral maps were generated for each paced activation sequence, 17 groups with nearly identical map features were visually selected, and a mean P-wave integral map was computed for each group. Supportive statistical analysis to corroborate qualitative group selection was performed by assessment of (1) intragroup pattern uniformity by use of jackknife correlation coefficient analysis of the integral maps contained in each group and (2) intergroup pattern variability by use of the calculation of cross correlations between the 17 mean integral maps. The spatial resolution of paced P-wave body surface mapping in the right atrium was obtained by estimating the area size of endocardial segments with nearly identical P-wave integral maps by use of a biplane fluoroscopic method to compute the three-dimensional position of each pacing site. The latter approach yielded a mean endocardial segment size of 3.5±2.9 cm2 (range, 0.79 to 10.75 cm2).

Conclusions—Use of the P-wave morphology on the 62-lead surface ECG in patients with normal biatrial anatomy allows separation of the origin of ectopic RA impulse formation into one of 17 different endocardial segments with an approximated area size of 3.5 cm2. This database of paced P-wave integral maps provides a versatile clinical tool to perform detailed noninvasive localization of right-sided atrial tachycardia before radiofrequency catheter ablation.


Key Words: mapping • morphogenesis • pacing




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