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首页> 外文期刊>American Journal of Physiology >Kinetics of cardiac muscle contraction and relaxation are linked and determined by properties of the cardiac sarcomere.
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Kinetics of cardiac muscle contraction and relaxation are linked and determined by properties of the cardiac sarcomere.

机译:心肌收缩和松弛的动力学是相互联系的,并由心肌肌小节的性质决定。

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摘要

The regulation of myocardial contraction and relaxation kinetics is currently incompletely understood. When the amplitude of contraction is increased via the Frank-Starling mechanism, the kinetics of the contraction slow down, but when the amplitude of contraction is increased with either an increase in heart rate or via beta-adrenergic stimulation, the kinetics speed up. It is also unknown how physiological mechanisms affect the kinetics of contraction versus those of relaxation. We investigated contraction-relaxation coupling in isolated trabeculae from the mouse and rat and stimulated them to contract at various temperatures, frequencies, preloads, and in the absence and presence of beta-adrenergic stimulation. In each muscle at least 16 different conditions were assessed, and the correlation coefficient of the speed of contraction and relaxation was very close (generally >0.98). Moreover, in all but one of the analyzed murine strains, the ratio of the minimum rate of the derivative of force development (dF/dt) over maximum dF/dt was not significantly different. Only in trabeculae isolated from myosin-binding protein-C mutant mice was this ratio significantly lower (0.61 +/- 0.07 vs. 0.84 +/- 0.02 in 11 other strains of mice). Within each strain, this ratio was unaffected by modulation of length, frequency, or beta-adrenergic stimulation. Rat trabeculae showed identical results; the balance between kinetics of contraction and relaxation was generally constant (0.85 +/- 0.04). Because of the great variety in underlying excitation-contraction coupling in the assessed strains, we concluded that contraction-relation coupling is a property residing in the cardiac sarcomere.
机译:目前尚不完全了解心肌收缩和舒张动力学的调节。当通过Frank-Starling机制增加收缩幅度时,收缩的动力学会减慢,但是当收缩幅度随心率增加或通过β-肾上腺素刺激而增加时,动力学会加快。还不知道生理机制如何影响收缩动力学和松弛动力学。我们研究了从小鼠和大鼠分离的小梁中的收缩松弛松弛偶联,并刺激它们在各种温度,频率,预负荷下以及在不存在和存在β-肾上腺素刺激的情况下收缩。在每只肌肉中至少评估了16种不同的条件,并且收缩和放松速度的相关系数非常接近(通常> 0.98)。此外,除了一种分析的鼠科菌株外,力发展导数的最小比率(dF / dt)与最大dF / dt的比率没有显着差异。仅在从肌球蛋白结合蛋白C突变小鼠中分离出的小梁中,该比率显着降低(其他11个小鼠品系中的比率为0.61 +/- 0.07,而0.84 +/- 0.02)。在每个菌株中,该比例不受长度,频率或β-肾上腺素刺激的调节的影响。大鼠小梁显示出相同的结果。收缩和松弛动力学之间的平衡通常是恒定的(0.85 +/- 0.04)。由于在评估的菌株中潜在的激发-收缩偶联的种类繁多,我们得出的结论是,收缩-偶联是心脏肌节中的一种特性。

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