Sleep-Disordered Breathing Destabilizes Ventricular Repolarization.

Soroosh Solhjoo, Mark C Haigney, Trishul Siddharthan, Abigail Koch, Naresh M Punjabi
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Abstract

Rationale: Sleep-disordered breathing (SDB) increases the risk of cardiac arrhythmias and sudden cardiac death.

Objectives: To characterize the associations between SDB, intermittent hypoxemia, and the beat-to-beat QT variability index (QTVI), a measure of ventricular repolarization lability associated with a higher risk for cardiac arrhythmias, sudden cardiac death, and mortality.

Methods: Three distinct cohorts were used for the current study. The first cohort, used for cross-sectional analysis, was a matched sample of 122 participants with and without severe SDB. The second cohort, used for longitudinal analysis, consisted of a matched sample of 52 participants with and without incident SDB. The cross-sectional and longitudinal cohorts were selected from the Sleep Heart Health Study participants. The third cohort comprised 19 healthy adults exposed to acute intermittent hypoxia and ambient air on two separate days. Electrocardiographic measures were calculated from one-lead electrocardiograms.

Results: Compared to those without SDB, participants with severe SDB had greater QTVI (-1.19 in participants with severe SDB vs. -1.43 in participants without SDB, P = 0.027), heart rate (68.34 vs. 64.92 beats/minute; P = 0.028), and hypoxemia burden during sleep as assessed by the total sleep time with oxygen saturation less than 90% (TST90; 11.39% vs. 1.32%, P < 0.001). TST90, but not the frequency of arousals, was a predictor of QTVI. QTVI during sleep was predictive of all-cause mortality. With incident SDB, mean QTVI increased from -1.23 to -0.86 over 5 years (P = 0.017). Finally, exposing healthy adults to acute intermittent hypoxia for four hours progressively increased QTVI (from -1.85 at baseline to -1.64 after four hours of intermittent hypoxia; P = 0.016).

Conclusions: Prevalent and incident SDB are associated with ventricular repolarization instability, which predisposes to ventricular arrhythmias and sudden cardiac death. Intermittent hypoxemia destabilizes ventricular repolarization and may contribute to increased mortality in SDB.

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睡眠呼吸紊乱使心室复极不稳定。
理由:睡眠呼吸障碍(SDB)会增加心律失常、猝死和全因死亡率的风险。目的:描述SDB、间歇性低氧血症和QT变异指数(QTVI)之间的关系,QT变异指数是衡量心室复极不稳定的指标,与心律失常、猝死和心血管死亡率的高风险相关。方法:使用来自三个队列的多导睡眠图:122名患有和不患有严重SDB的参与者的匹配样本,52名患有和没有发生SDB的参与者,以及19名在两天内暴露于间歇性缺氧和环境空气的健康成年人的队列。心电图测量是根据单导联心电图计算的。测量和主要结果:与没有SDB的参与者相比,患有严重SDB的参与者具有更大的QTVI(-1.19 vs.-1.43,P=0.027)、心率(68.34 vs.64.92次/分;P=0.028)、,通过血氧饱和度低于90%的总睡眠时间来评估睡眠期间的低氧血症负担(TST90;11.39%对1.32%,P90,但不是觉醒频率,是QTVI的预测因素。睡眠期间的心率和QTVI可预测全因死亡率。在发生SDB的队列中,平均QTVI在5年内从-1.23增加到-0.86(P=0.017)。最后,在健康成年人队列中,暴露于间歇性缺氧4小时会增加QTVI(-1.85 vs.-1.64;P=0.016)。结论:常见和偶发的SDB与心室复极不稳定有关,后者易导致室性心律失常和心源性猝死。间歇性低氧血症可使心室复极不稳定,并可能介导SDB死亡率的增加。
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