医学
内科学
心脏病学
再入
致心律失常性右心室发育不良
室性心动过速
心肌病
射血分数
心内膜
心室流出道
心动过速
心力衰竭
作者
Ruhong Jiang,Takuro Nishimura,Andrew D. Beaser,Zaid Aziz,Gaurav A. Upadhyay,Dalise Y. Shatz,Hemal M. Nayak,Hongtao Liao,Xianzhang Zhan,Fa Po Chung,Yumei Xue,Shulin Wu,Roderick Tung
出处
期刊:Heart Rhythm
[Elsevier]
日期:2021-01-30
卷期号:18 (6): 916-925
被引量:8
标识
DOI:10.1016/j.hrthm.2021.01.028
摘要
While advances in the characterization of the structural substrate in arrhythmogenic right ventricular cardiomyopathy (ARVC) have been made, the ventricular tachycardia (VT) circuit remains incompletely described.The purpose of this study was to delineate the reentrant VT circuit with simultaneous epicardial and endocardial mapping (SEEM) in ARVC.Twenty-three consecutive patients with ARVC and VT underwent SEEM at 4 centers between 2014 and 2020. Retrospective analysis was performed on combined isochronal activation maps.Of the 30 VT circuits, 24 were delineated with SEEM (956 [341-1843] endocardial points and 1763 [882-3054] epicardial points). The apex and outflow tract rarely harbored VT circuits, with 50% distributed in the inferior wall and 43% in the free wall. The entire tachycardia cycle length was recorded from the epicardium in 71% of circuits. In all circuits, a large proportion of the tachycardia cycle length was recorded from the epicardium relative to the endocardium. Localized epicardial reentry was observed in 35% of patients (14 mm × 15 mm), which was associated with smaller endocardial low voltage area (39 cm2 vs 104 cm2; P = .002) and preserved right ventricular ejection fraction (35% vs 25%; P = .046) compared with those with larger circuit dimensions. Seventy percent of termination sites were achieved from the epicardium.High-resolution recordings from both myocardial surfaces confirm a consistent predominance of epicardial participation during reentry in ARVC. Only the perivalvular inflow region of the "triangle of dysplasia" had a strong propensity to harbor VT circuits, with the greatest proportion located in the inferior wall. Localized epicardial reentry may be a manifestation of earlier stage disease with a relative paucity of endocardial substrate.
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