首页> 外文期刊>Cell Calcium: The International Interdisciplinary Forum for Research on Calcium >Comparison of the T-tubule system in adult rat ventricular and atrial myocytes, and its role in excitation-contraction coupling and inotropic stimulation.
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Comparison of the T-tubule system in adult rat ventricular and atrial myocytes, and its role in excitation-contraction coupling and inotropic stimulation.

机译:成年大鼠心室和心房肌细胞T管系统的比较,及其在兴奋收缩耦合和正性肌力刺激中的作用。

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摘要

Narrow, tubular, inward projections of the sarcolemma ('T-tubules') are an established feature of adult mammalian ventricular myocytes that enables them to generate the whole-cell Ca2+ transients and produce coordinated contraction. Loss of T-tubules can occur during ageing and under pathological conditions, leading to altered cardiac excitation-contraction coupling. In contrast to adult ventricular cells, atrial myocytes do not generally express an extensive T-tubule system at any stage of development, and therefore rely on Ca2+ channels around their periphery for the induction of Ca2+ signalling and excitation-contraction coupling. Consequently, the characteristics of systolic Ca2+ signals in adult ventricular and atrial myocytes are temporally and spatially distinct. However, although atrial myocytes do not have the same regularly spaced convoluted T-tubule structures as adult ventricular cells, it has been suggested that a proportion of adult atrial cells have a more rudimentary tubule system. We examined the structure and function of these atrial tubules, and explored their impact on the initiation and recovery of Ca2+ signalling in electrically paced myocytes. The atrial responses were compared to those in adult ventricular cells that had intact T-tubules, or that had been chemically detubulated. We found that tubular structures were present in a significant minority of adult atrial myocytes, and were unlike the T-tubules in adult ventricular cells. In those cells where they were present, the atrial tubules significantly altered the on-set, amplitude, homogeneity and recovery of Ca2+ transients. The properties of adult atrial myocyte Ca2+ signals were different from those in adult ventricular cells, whether intact or detubulated. Excitation-contraction coupling in detubulated adult ventricular myocytes, therefore, does not approximate to atrial signalling, even though Ca2+ signals are initiated in the periphery of the cells in both of these situations. Furthermore, inotropic responses to endothelin-1 were entirely dependent on T-tubules in adult ventricular myocytes, but not in atrial cells. Our data reveal that that the T-tubules in atrial cells impart significant functional properties, but loss of these tubular membranes does not affect Ca2+ signalling as dramatically as detubulation in ventricular myocytes.
机译:肌膜的狭窄,管状,向内投影(“ T型小管”)是成年哺乳动物心室肌细胞的既定特征,可使它们产生全细胞Ca2 +瞬变并产生协调的收缩。 T管的丢失可能会在衰老过程中和在病理条件下发生,从而导致心脏兴奋-收缩耦合改变。与成年心室细胞相反,心房肌细胞通常在任何发育阶段均不表达广泛的T管系统,因此依赖于其周围的Ca2 +通道来诱导Ca2 +信号传导和激发-收缩偶联。因此,成人心室和心房肌细胞中收缩期Ca2 +信号的特征在时间和空间上是不同的。然而,尽管心房肌细胞不具有与成年心室细胞相同的规则间隔的回旋T形管结构,但是已经建议一定比例的成年心房细胞具有更基本的肾小管系统。我们检查了这些心房小管的结构和功能,并探讨了它们对电起搏的心肌细胞中Ca2 +信号传导和恢复的影响。将心房反应与具有完整T形管或已化学脱管的成年心室细胞的反应进行了比较。我们发现肾小管结构存在于成年心房肌细胞的显着少数,并且不像成年心室细胞中的T管。在存在它们的那些细胞中,心房小管显着改变了Ca2 +瞬变的发作,幅度,均一性和恢复。成年心房肌细胞Ca2 +信号的特性与成年心室细胞的特性不同,无论是完整的还是拔管的。因此,即使在这两种情况下都在细胞周围引发了Ca2 +信号,成管后的成年心室肌细胞中的兴奋-收缩偶联也不近似于心房信号。此外,对内皮素-1的正性肌力反应完全依赖于成年心室肌细胞中的T-管,但不依赖于心房细胞。我们的数据表明,心房中的T管具有显着的功能特性,但是这些肾小管膜的丢失不会像心室肌细胞中的小管一样显着影响Ca2 +信号传导。

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