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收缩期骨骼肌和心肌细胞中的钙离子空间分布

Spatial Ca(2+) distribution in contracting skeletal and cardiac muscle cells.

作者信息

Zoghbi M E, Bolaños P, Villalba-Galea C, Marcano A, Hernández E, Fill M, Escobar A L

机构信息

Instituto Venezolano de Investigaciones Científicas, Pipe, Venezuela.

出版信息

Biophys J. 2000 Jan;78(1):164-73. doi: 10.1016/S0006-3495(00)76582-9.

Abstract

The spatiotemporal distribution of intracellular Ca(2+) release in contracting skeletal and cardiac muscle cells was defined using a snapshot imaging technique. Calcium imaging was performed on intact skeletal and cardiac muscle cells during contractions induced by an action potential (AP). The sarcomere length of the skeletal and cardiac cells was approximately 2 micrometer. Imaging Rhod-2 fluorescence only during a very brief (7 ns) snapshot of excitation light minimized potential image-blurring artifacts due to movement and/or diffusion. In skeletal muscle cells, the AP triggered a large fast Ca(2+) transient that peaked in less than 3 ms. Distinct subsarcomeric Ca(2+) gradients were evident during the first 4 ms of the skeletal Ca(2+) transient. In cardiac muscle, the AP-triggered Ca(2+) transient was much slower and peaked in approximately 100 ms. In contrast to the skeletal case, there were no detectable subsarcomeric Ca(2+) gradients during the cardiac Ca(2+) transient. Theoretical simulations suggest that the subsarcomeric Ca(2+) gradients seen in skeletal muscle were detectable because of the high speed and synchrony of local Ca(2+) release. Slower asynchronous recruitment of local Ca(2+) release units may account for the absence of detectable subsarcomeric Ca(2+) gradients in cardiac muscle. The speed and synchrony of local Ca(2+) gradients are quite different in AP-activated contracting cardiac and skeletal muscle cells at normal resting sarcomere lengths.

摘要

利用一种快照成像技术确定了收缩骨骼肌和心肌细胞内钙离子(Ca(2+))释放的时空分布。在动作电位(AP)诱导的收缩过程中,对完整的骨骼肌和心肌细胞进行钙成像。骨骼肌和心肌细胞的肌节长度约为2微米。仅在激发光的极短(7纳秒)快照期间对罗丹明2荧光进行成像,可将由于移动和/或扩散导致的潜在图像模糊伪影降至最低。在骨骼肌细胞中,动作电位触发了一个大的快速Ca(2+)瞬变,在不到3毫秒内达到峰值。在骨骼肌Ca(2+)瞬变的前4毫秒内,明显可见不同的肌节下Ca(2+)梯度。在心肌中,动作电位触发的Ca(2+)瞬变更慢,在约100毫秒内达到峰值。与骨骼肌情况不同,在心肌Ca(2+)瞬变期间未检测到肌节下Ca(2+)梯度。理论模拟表明,骨骼肌中可见的肌节下Ca(2+)梯度是由于局部Ca(2+)释放的高速和同步性而可检测到的。局部Ca(2+)释放单位较慢的异步募集可能解释了心肌中未检测到肌节下Ca(2+)梯度的原因。在正常静息肌节长度下,动作电位激活的收缩心肌和骨骼肌细胞中局部Ca(2+)梯度的速度和同步性有很大差异。

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