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维拉帕米对急性心肌梗死后心率变异性指标的影响。

Effects of verapamil on indexes of heart rate variability after acute myocardial infarction.

作者信息

Pinar E, García-Alberola A, Llamas C, Vicente T, López-Candel J, Rojo J L, Fernández R, Valdés M

机构信息

Department of Cardiology, General Hospital of the University of Murcia, Spain.

出版信息

Am J Cardiol. 1998 May 1;81(9):1085-9. doi: 10.1016/s0002-9149(98)00128-3.

Abstract

In patients with previous myocardial infarction (MI), depressed heart rate variability (HRV) may reflect a reduction in vagal activity and lead to cardiac electrical instability. Interventions designed to increase HRV may be of clinical interest. Data on the effects of calcium antagonists on HRV in post-MI patients are very limited. The aim of our study was to assess the effects of verapamil on HRV and on the sympathovagal balance after MI. Fifty consecutive patients with a first MI, stable sinus rhythm, and left ventricular ejection fraction >0.40 were studied. Each patient underwent two 24-hour Holter recordings, 1 at baseline and another after 4 days of treatment with verapamil retard (180 mg 2 times daily). Time and frequency domain parameters of HRV were analyzed. All time domain measurements increased significantly after verapamil: the standard deviation of all NN intervals (SDNN) from 87.1 +/- 31.4 to 98.1 +/- 30.3 ms (p <0.05) and the log-transformed percentage of pairs of adjacent NN intervals that differ >50 ms (pNN50) from 0.57 +/- 0.42 to 0.76 +/- 0.45 (p <0.01). The standard deviation of the averages of RR interevals (SDANN) (75.9 +/- 30.1 vs 86.3 +/- 29.4 ms, p <0.05), root-mean-square of successive differences between RR intervals (rMSSD) (23.0 +/- 11.7 and 28.1 +/- 13.1 ms, p <0.01), and the triangular HRV index (28.3 +/- 9.6 vs 23.4 +/- 8.6, p <0.001) also increased. A significant inverse correlation was found between improvement in HRV indexes induced by verapamil and baseline values. Spectral analysis showed a significant increase in high-frequency power of 58.5% without changes in low and very low components. With normalized units, significant reductions in low-frequency power and low- to high-frequency ratio were observed. Diabetic patients did not show any significant changes in HRV on administration of verapamil. These findings indicate that verapamil, administered during the subacute phase of MI, improves both global and short-period indexes of HRV and induces a shift in the sympathetic-parasympathetic interaction toward vagal predominance. This effect may contribute to an explanation of the beneficial effects of verapamil that have been reported in post-MI patients.

摘要

在既往有心肌梗死(MI)的患者中,心率变异性(HRV)降低可能反映迷走神经活动减弱并导致心脏电活动不稳定。旨在增加HRV的干预措施可能具有临床意义。关于钙拮抗剂对心肌梗死后患者HRV影响的数据非常有限。我们研究的目的是评估维拉帕米对心肌梗死后HRV及交感-迷走神经平衡的影响。对50例首次发生心肌梗死、窦性心律稳定且左心室射血分数>0.40的连续患者进行了研究。每位患者进行两次24小时动态心电图记录,一次在基线时,另一次在服用缓释维拉帕米(每日2次,每次180mg)4天后。分析了HRV的时域和频域参数。服用维拉帕米后,所有时域测量值均显著增加:所有NN间期的标准差(SDNN)从87.1±31.4ms增至98.1±30.3ms(p<0.05),相邻NN间期差值>50ms的对数转换百分比(pNN50)从0.57±0.42增至0.76±0.45(p<0.01)。RR间期平均值的标准差(SDANN)(75.9±30.1对86.3±29.4ms,p<0.05)、RR间期连续差值的均方根(rMSSD)(23.0±11.7和28.1±13.1ms,p<0.01)以及三角HRV指数(28.3±9.6对23.4±8.6,p<0.001)也增加。发现维拉帕米诱导的HRV指标改善与基线值之间存在显著负相关。频谱分析显示高频功率显著增加58.5%,低频和极低频成分无变化。以标准化单位表示,低频功率和低频与高频比值显著降低。糖尿病患者服用维拉帕米后HRV未显示任何显著变化。这些发现表明,在心肌梗死亚急性期给予维拉帕米可改善HRV的整体和短期指标,并使交感-副交感神经相互作用向迷走神经占优势转变。这一效应可能有助于解释在心肌梗死后患者中报道的维拉帕米的有益作用。

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