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Selective sinoatrial node optical mapping to investigate the mechanism of sinus rate acceleration

机译:选择性窦房结光学测绘研究窦速度加速机制

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摘要

Studies using isolated sinoatrial node (SAN) cells indicate that rhythmic spontaneous sarcoplasmic reticulum Ca release (Ca clock) plays an important role in SAN automaticity. However, it is difficult to translate these findings into intact SAN because the SAN is embedded in the right atrium (RA). Cross contamination of the optical signals between SAN and RA prevented the definitive testing of Ca clock hypothesis in intact SAN. We use a novel approach to selectively map intact SAN to examine the Ca clock function in intact RA. We simultaneously mapped intracellular Ca (Cai) and membrane potential (Vm) in 7 isolated, Langendorff perfused normal canine RA. Electrical conduction from the SAN to RA was inhibited with high potassium (10 mmol/L) Tyrode's solution, allowing selective optical mapping of Vm and Cai of the SAN. Isoproterenol (ISO, 0.03 umol/L) decreased cycle length of the sinus beats from 586±17 ms at baseline to 366±32 ms, and shifted the leading pacemaker site from the middle or inferior SAN to the superior SAN in all RAs. The Cai upstroke preceded the Vm in the leading pacemaker site by up to 18±2 ms. ISO-induced changes to SAN were inhibited by ryanodine (3 umol/L), but not ZD7288 (3 umol/L), a selective If blocker. We conclude that a high extracellular potassium concentration results in intermittent SAN-RA conduction block, allowing selective optical mapping of the intact SAN. Acceleration of Ca cycling in the superior SAN underlies the mechanism of sinus tachycardia during sympathetic stimulation.
机译:使用隔离的窦房结(SAN)细胞进行的研究表明,节奏性自发性肌浆网Ca释放(Ca Clock)在SAN自动化中起重要作用。但是,由于将SAN嵌入右心房(RA)中,因此很难将这些发现转换为完整的SAN。 SAN和RA之间的光信号交叉污染阻止了对完整SAN中Ca时钟假设的确定性测试。我们使用一种新颖的方法来选择性地映射完整的SAN,以检查完整RA中的Ca时钟功能。我们同时绘制了7个孤立的Langendorff灌注正常犬RA中的细胞内Ca(Cai)和膜电位(Vm)的图。高钾(10 mmol / L)的Tyrode溶液抑制了从SAN到RA的导电,从而可以选择性地绘制SAN的Vm和Cai。异丙肾上腺素(ISO,0.03 umol / L)将窦性搏动的周期长度从基线的586±17 ms减少到366±32 ms,并且将所有心脏起搏器的主要部位从中级或下级SAN转移到了上级SAN。在领先的起搏器部位,蔡氏上风先于Vm达18±2 ms。 ISO诱导的SAN改变受到雷诺定(3 umol / L)的抑制,但未被ZD7288(3 umol / L)(一种选择性的If阻滞剂)抑制。我们得出的结论是,细胞外钾离子浓度高会导致SAN-RA传导阻滞间歇性发生,从而允许对完整SAN进行选择性光学定位。上级SAN中Ca循环的加速是交感神经刺激期间窦性心动过速的机制的基础。

著录项

  • 来源
    《Photonic therapeutics and diagnostics VII 》|2011年|p.78832Z.1-78832Z.7|共7页
  • 会议地点 San Francisco CA(US)
  • 作者单位

    Krannert Institute of Cardiology and the Division of Cardiology, Department of Medicine Indiana University School of Medicine, Indianapolis, Indiana, USA;

    Krannert Institute of Cardiology and the Division of Cardiology, Department of Medicine Indiana University School of Medicine, Indianapolis, Indiana, USA;

    Krannert Institute of Cardiology and the Division of Cardiology, Department of Medicine Indiana University School of Medicine, Indianapolis, Indiana, USA;

    Krannert Institute of Cardiology and the Division of Cardiology, Department of Medicine Indiana University School of Medicine, Indianapolis, Indiana, USA;

  • 会议组织
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医用物理学 ;
  • 关键词

    calcium; nervous system; sympathetic; sarcoplasmic reticulum; sinoatrial node;

    机译:钙;神经系统;交感;肌浆网;窦房结;

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