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摄食时间对小鼠的影响揭示了心肌细胞生物钟机制在限制 QT 间期延长中的作用。

Timing of food intake in mice unmasks a role for the cardiomyocyte circadian clock mechanism in limiting QT-interval prolongation.

机构信息

Department of Physiology, University of Kentucky, Lexington, Kentucky, USA.

Internal Medicine, Pulmonary, University of Kentucky, Lexington, Kentucky, USA.

出版信息

Chronobiol Int. 2022 Apr;39(4):525-534. doi: 10.1080/07420528.2021.2011307. Epub 2021 Dec 7.

Abstract

Cardiac electrophysiological studies demonstrate that restricting the feeding of mice to the light cycle (time restricted feeding or TRF) causes a pronounced change in heart rate and ventricular repolarization as measured by the RR- and QT-interval, respectively. TRF slows heart rate and shifts the peak (acrophase) of the day/night rhythms in the RR- and QT-intervals from the light to the dark cycle. This study tested the hypothesis that these changes in cardiac electrophysiology are driven by the cardiomyocyte circadian clock mechanism. We determined the impact that TRF had on RR- and QT-intervals in control mice or mice that had the cardiomyocyte circadian clock mechanism disrupted by inducing the deletion of in adult cardiomyocytes (iCSΔ mice). In control and iCSΔ mice, TRF increased the RR-intervals measured during the dark cycle and shifted the acrophase of the day/night rhythm in the RR-interval from the light to the dark cycle. Compared to control mice, TRF caused a larger prolongation of the QT-interval measured from iCSΔ mice during the dark cycle. The larger QT-interval prolongation in the iCSΔ mice caused an increased mean and amplitude in the day/night rhythm of the QT-interval. There was not a difference in the TRF-induced shift in the day/night rhythm of the QT-interval measured from control or iCSΔ mice. We conclude that the cardiomyocyte circadian clock does not drive the changes in heart rate or ventricular repolarization with TRF. However, TRF unmasks an important role for the cardiomyocyte circadian clock to prevent excessive QT-interval prolongation, especially at slow heart rates.

摘要

心脏电生理研究表明,限制小鼠在光照周期内进食(限时喂养或 TRF)会导致心率和心室复极分别通过 RR 间期和 QT 间期明显改变。TRF 会降低心率,并将 RR 间期和 QT 间期中日/夜节律的峰值(高峰相位)从光照周期转移到暗周期。本研究检验了心脏电生理学变化是由心肌细胞生物钟机制驱动的假说。我们确定了 TRF 对对照小鼠或通过诱导成年心肌细胞中缺失(iCSΔ 小鼠)破坏心肌细胞生物钟机制的小鼠 RR 间期和 QT 间期的影响。在对照和 iCSΔ 小鼠中,TRF 增加了暗周期测量的 RR 间期,并将 RR 间期中日/夜节律的高峰相位从光照周期转移到暗周期。与对照小鼠相比,TRF 导致暗周期中从 iCSΔ 小鼠测量的 QT 间期延长更大。iCSΔ 小鼠中较大的 QT 间期延长导致 QT 间期的日/夜节律的平均和幅度增加。从对照或 iCSΔ 小鼠测量的 QT 间期的日/夜节律中,TRF 诱导的变化没有差异。我们得出结论,心肌细胞生物钟不会驱动 TRF 引起的心率或心室复极变化。然而,TRF 揭示了心肌细胞生物钟的一个重要作用,可防止 QT 间期过度延长,尤其是在心率较慢时。

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