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首页> 外文期刊>American Journal of Physiology >Myocardial ischemia-reperfusion damage impacts occurrence of ventricular fibrillation in dogs.
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Myocardial ischemia-reperfusion damage impacts occurrence of ventricular fibrillation in dogs.

机译:心肌缺血-再灌注损伤影响犬心室纤颤的发生。

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摘要

To define the relationship between ischemia-reperfusion-induced myocardial damage (IRD) and the occurrence of ventricular tachycardia (VT) and fibrillation (VF), we studied 23 dogs with a three-dimensional activation mapping system. Left anterior descending (LAD) coronary artery occlusion and reperfusion were performed while recording electrograms during VF and atrial pacing. Prior nonischemic sites showing IRD, defined as at least 10% loss of electrogram voltage after reperfusion, had the longest ventricular effective refractory periods (ERPs). IRD sites also occurred more frequently in dogs with reperfusion VF (44 +/- 2 sites, P < 0.01) compared with dogs with VT (18 +/- 5 sites) and no VT (16 +/- 3 sites). In dogs (n = 3) with 3 h of reperfusion, 95% of IRD sites still had lower voltage than those recorded during occlusion. Activation mapping of the first eight complexes of VF had Purkinje or endocardial focal origin in 57%, and complexes originated from IRD sites in 28%. In contrast, dogs with onlyreperfusion VT also had Purkinje or endocardial focal origin in 79%, but only 5% (P < 0.01 vs. VF dogs) of the sites of origin had IRD. Therefore, dogs with reperfusion VF had more IRD sites where the ERP was longest, and more focal ventricular complexes originated from IRD sites, indicating that IRD may be one important factor in the occurrence of VF during reperfusion.
机译:为了定义缺血再灌注引起的心肌损伤(IRD)与室性心动过速(VT)和心律颤动(VF)的发生之间的关系,我们用三维激活映射系统研究了23只狗。在记录心电图和心房起搏期间的电描记图时,进行左前降(LAD)冠状动脉闭塞和再灌注。先前显示IRD的非缺血性部位(定义为再灌注后至少10%的电图电压损失)具有最长的心室有效不应期(ERP)。与具有VT(18 +/- 5个位点)和没有VT(16 +/- 3个位点)的狗相比,具有再灌注VF的狗(44 +/- 2个位点,P <0.01)的IRD部位也更常见。在再灌注3 h的狗(n = 3)中,仍有95%的IRD部位的电压低于闭塞期间记录的电压。 VF的前八个复合物的激活图谱显示有57%的是Purkinje或心内膜局灶性起源,而来自IRD部位的复合物则为28%。相比之下,仅再灌注VT的狗也有Purkinje或心内膜局灶性起源,占79%,但是只有5%(与VF狗相比P <0.01)有IRD。因此,具有再灌注VF的狗在ERP最长的地方有更多的IRD部位,并且更多的局灶性心室复合体起源于IRD部位,这表明IRD可能是再灌注期间VF发生的重要因素之一。

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