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Disease-Specific Electrocardiographic Lead Positioning for Early Detection of Arrhythmogenic Right Ventricular Cardiomyopathy

机译:疾病特异性心电图铅定位,用于早期检测心律源右心室心肌病

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Arrhythmogenic right ventricular cardiomyopathy (ARVC) is characterized by replacement of cardiomyocytes by fibrofatty tissue which can lead to ventricular arrhythmias, heart failure or sudden cardiac death. Genetic defects in desmosomal proteins, as plakophilin-2 (PKP2), are known to contribute to disease development. Current electrocardiographic (ECG) criteria for ARVC diagnosis only focus on right precordial leads, but sensitivity of current depolarization criteria is limited. This study aimed to identify additional depolarization criteria with most optimal lead configurations for early detection of ARVC in PKP2 pathogenic mutation carriers. In PKP2-positive ARVC patients (n=7), PKP2 pathogenic variant carriers (n=16) and control subjects without structural heart disease (n=9), 67-lead body surface potential maps (BSPM) were obtained. Terminal QRS-integrals were determined and quantitatively compared to controls using departure mapping. Significantly different terminal QRS-integrals were identified in lead 34 (conventional V3), 40 and 41 (conventional V4). To conclude, a clear distinction between ARVC patients, asymptomatic mutation carriers and healthy controls was observed.
机译:心血生右心室心肌病(ARVC)的特征是通过纤维脂肪组织替代心肌细胞,这可以导致心律失常心律失常,心力衰竭或突然的心脏死亡。已知丙蛋白蛋白(PKP2)中的遗传缺陷是有助于疾病发育。 ARVC诊断的当前心电图(ECG)标准仅关注右前方引线,但电流去极化标准的敏感性有限。该研究旨在识别具有最佳铅型促进抗原血管生成突变载体中ARVC的最佳铅构型的额外去极化标准。在PKP2阳性ARVC患者(n = 7)中,获得PKP2致病变体载体(N = 16)和没有结构心脏病(n = 9),67-铅体表面潜在图(BSPM)的对照受试者。与使用脱映映射的控制相比,确定和定量终端QRS积分。在引线34(常规V3),40和41(常规V4)中鉴定出显着不同的终端QRS-积分。为了得出结论,观察到ARVC患者,无症状突变携带者和健康对照之间的明确区别。

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