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首页> 外文期刊>Journal of Muscle Research and Cell Motility >Cardiotonic bipyridine amrinone slows myosin-induced actin filament sliding at saturating [MgATP]
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Cardiotonic bipyridine amrinone slows myosin-induced actin filament sliding at saturating [MgATP]

机译:强直性联吡啶氨力农酮可减慢肌球蛋白诱导的肌动蛋白丝饱和时的滑动[MgATP]

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摘要

Previously reported effects of amrinone on skeletal muscle function suggest that the drug reduces the rate constant of myosin cross-bridge dissociation. We have used the in vitro motility assay to further elucidate the mechanism underlying this effect and to aid these studies a new, improved, filament tracking software was developed in the Matlab™ environment. The experiments were carried out at 30°C using heavy meromyosin from fast rabbit muscle and rhodamine–phalloidin labeled actin filaments. A slowing effect of amrinone on filament sliding velocity at 1mM MgATP was observed at drug concentrations >0.3 mM. This effect showed signs of saturation at the highest drug concentrations (1–2 mM) that could be readily tested. The sliding velocity exhibited hyperbolic dependence on [MgATP] with a V max of 7.2 ± 0.9 μm/s and a K M of 0.18 ± 0.02 mM. Amrinone (1 mM) reduced V max by 32 ± 5% (P < 0.01) and K M by 42 ± 8% (P < 0.05; n = 4). These results are accounted for in the most straightforward way by a model where amrinone acts directly on the actomyosin system and reduces the rate constant of MgADP release. Such a well-defined effect on the myosin cross-bridge cycle makes the drug a potentially useful pharmacological tool for further studies of myosin function both in vitro and in the ordered filament array of a living muscle fiber.
机译:先前报道的氨力农对骨骼肌功能的影响表明该药物降低了肌球蛋白跨桥解离的速率常数。我们已经使用体外运动测定法进一步阐明了这种作用的潜在机制,并为协助这些研究,在Matlab™环境中开发了一种新的,改进的细丝跟踪软件。实验是使用快速兔肌肉中的重肌球蛋白和若丹明-鬼笔环肽标记的肌动蛋白丝在30°C进行的。在> 0.3 mM的药物浓度下,观察到氨力农对细丝滑动速度的影响为1mM MgATP。这种作用在最高药物浓度(1-2 mM)下显示出饱和迹象,可以容易地进行测试。滑动速度表现出对[MgATP]的双曲线依赖性,V max 为7.2±0.9μm/ s,K M 为0.18±0.02 mM。氨力农(1 mM)将V max 降低32±5%(P <0.01),将K M 降低42±8%(P <0.05; n = 4)。这些结果是模型最直接的方法,其中氨力农直接作用于放线菌素系统并降低MgADP释放的速率常数。这种对肌球蛋白跨桥循环的明确作用使该药物成为潜在的有用的药理学工具,可用于进一步研究肌球蛋白的功能,无论是在体外还是在活肌纤维的有序细丝阵列中。

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    J. Klinth; A. Arner; A. Månsson;

  • 作者单位

    Department of Chemistry and Biomedical Sciences University of Kalmar;

    Department of Physiological Sciences University of Lund;

    Department of Chemistry and Biomedical Sciences University of Kalmar;

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