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离体血液灌注猪心脏心室颤动期间细胞内钙离子动力学与波破碎之间的时空关系。

Spatiotemporal relationship between intracellular Ca2+ dynamics and wave fragmentation during ventricular fibrillation in isolated blood-perfused pig hearts.

作者信息

Warren Mark, Huizar José F, Shvedko Alexander G, Zaitsev Alexey V

机构信息

Nora Eccles Harrison CVRTI, University of Utah, Salt Lake City, UT 84112-5000, USA.

出版信息

Circ Res. 2007 Oct 26;101(9):e90-101. doi: 10.1161/CIRCRESAHA.107.162735. Epub 2007 Oct 11.

Abstract

Normal "master-slave" relationship between the action potential (AP) and intracellular Ca2+ transient (Ca(i)T) is sometimes altered during ventricular fibrillation (VF). The nature of AP/Ca(i)T dissociation during VF and its role in inducing wavebreaks (WBs) remain unclear. We simultaneously mapped AP (RH237) and Ca(i)T (Rhod-2) during VF in blood-perfused pig hearts. We computed AP and Ca(i)T dominant frequency (DF) and Ca(i)T delay in each AP cycle. We identified WBs as singularity points in AP phase movies and sites of conduction block (CB) as sites where an AP wavefront failed to propagate. We analyzed spatiotemporal relationship between abnormal AP/Ca(i)T sequences and CB sites. We used a calcium chelator (BAPTA-AM) to abolish Ca(i)T and test its involvement in WB formation. During VF, the DF difference between AP and Ca(i)T was <10% of the respective values in 95% of pixels, and 80% of all Ca(i)T upstrokes occurred during the initial 25% of the excitation cycle. Aberrant sequences of AP and Ca(i)T occurred almost exclusively near CB sites but could be traced to normal wavefront sequences away from CB sites. Thus, apparent AP/Ca(i)T dissociation was largely attributable to spatial uncertainty of the absolute position of block of each wave. BAPTA-AM reduced Ca(i)T amplitude to 30.5+/-12.9% of control and the DF of AP from 12.2+/-1.6 to 10.4+/-1.3 Hz (P<0.01), but did not significantly alter WB incidence (0.76+/-0.19 versus 0.72+/-0.19 SP/mm2). These results do not support presence of spontaneous, non-voltage-gated Ca(i)Ts during VF and suggest that AP/Ca(i)T dissociation is a consequence rather than a cause of wave fragmentation.

摘要

在心室颤动(VF)期间,动作电位(AP)与细胞内Ca2+瞬变(Ca(i)T)之间正常的“主 - 从”关系有时会发生改变。VF期间AP/Ca(i)T解离的本质及其在引发波破碎(WB)中的作用仍不清楚。我们在血液灌注的猪心脏VF期间同时绘制了AP(RH237)和Ca(i)T(Rhod - 2)。我们计算了每个AP周期中AP和Ca(i)T的主导频率(DF)以及Ca(i)T延迟。我们将WB识别为AP相位电影中的奇点,将传导阻滞(CB)位点识别为AP波前未能传播的位点。我们分析了异常AP/Ca(i)T序列与CB位点之间的时空关系。我们使用钙螯合剂(BAPTA - AM)消除Ca(i)T并测试其在WB形成中的作用。在VF期间,AP和Ca(i)T之间的DF差异在95%的像素中小于各自值的10%,并且所有Ca(i)T上升支的80%发生在兴奋周期的最初25%期间。AP和Ca(i)T的异常序列几乎仅出现在CB位点附近,但可以追溯到远离CB位点的正常波前序列。因此,明显的AP/Ca(i)T解离很大程度上归因于每个波阻滞绝对位置的空间不确定性。BAPTA - AM将Ca(i)T幅度降低至对照的30.5±12.9%,AP的DF从12.2±1.6降至10.4±1.3 Hz(P<0.01),但并未显著改变WB发生率(0.76±0.19对0.72±0.19个奇点/平方毫米)。这些结果不支持VF期间存在自发性、非电压门控Ca(i)T,并表明AP/Ca(i)T解离是波破碎的结果而非原因。

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