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舒张期心脏收缩蛋白的状态。

The state of cardiac contractile proteins during the diastolic phase.

作者信息

Matsubara I, Yagi N, Endoh M

出版信息

Jpn Circ J. 1982 Jan;46(1):44-8. doi: 10.1253/jcj.46.44.

Abstract

The molecular events underlying contraction and relaxation of heart muscle were studied by the X-ray diffraction method. In quiescent heart muscle most myosin heads were in the vicinity of the thick filaments. When heart muscle contracted, myosin heads moved to the vicinity of the thin filaments to react with actin. On relaxation of muscle, myosin heads returned to the thick filaments. However, in cyclically contracting heart muscle a significant fraction of myosin heads remained in the vicinity of the thin filaments until the end of the diastolic phase. Therefore, the molecular state during the diastolic phase was considerably different from that in the quiescent state. Paired-pulse stimulation, which enhanced the tension development, increased the number of myosin heads near the thin filaments not only during the systolic phase but also during the diastolic phase. Thus the diastolic molecular state was modified by inotropic intervention. These findings suggest that the diastolic phase should be regarded as a dynamic phase rather than a static phase.

摘要

采用X射线衍射法研究了心肌收缩和舒张的分子机制。在静息心肌中,大多数肌球蛋白头部位于粗肌丝附近。当心肌收缩时,肌球蛋白头部移动到细肌丝附近与肌动蛋白反应。肌肉舒张时,肌球蛋白头部回到粗肌丝。然而,在周期性收缩的心肌中,相当一部分肌球蛋白头部在舒张期末期之前一直留在细肌丝附近。因此,舒张期的分子状态与静息状态有很大不同。双脉冲刺激可增强张力发展,不仅在收缩期而且在舒张期都增加了细肌丝附近肌球蛋白头部的数量。因此,变力干预改变了舒张期的分子状态。这些发现表明,舒张期应被视为一个动态阶段而非静态阶段。

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