使用吡啶斯的明进行胆碱能刺激可减少心力衰竭患者的室性心律失常并增强心率变异性。

Cholinergic stimulation with pyridostigmine reduces ventricular arrhythmia and enhances heart rate variability in heart failure.

作者信息

Behling Alice, Moraes Ruy S, Rohde Luis E, Ferlin Elton L, Nóbrega Antonio C L, Ribeiro Jorge P

机构信息

Division of Cardiology, Hospital de Clínicas de Porto Alegre, Porto Alegre, Brazil.

出版信息

Am Heart J. 2003 Sep;146(3):494-500. doi: 10.1016/S0002-8703(03)00319-3.

DOI:10.1016/S0002-8703(03)00319-3

PMID:12947369

Abstract

BACKGROUND

Increased ventricular arrhythmia density and reduced heart rate variability are associated with risk of death in patients with heart failure. Cholinesterase inhibition with pyridostigmine bromide increases heart rate variability in normal subjects, but its effect on patients with heart failure is unknown. In this study, we tested the hypothesis that short-term administration of pyridostigmine bromide, a cholinesterase inhibitor, reduces ventricular arrhythmia density and increases heart rate variability in patients with congestive heart failure.

METHODS

Patients with heart failure and in sinus rhythm participated in a double-blind, cross-over protocol, randomized for placebo and pyridostigmine (30 mg orally 3 times daily for 2 days). Twenty-four hour electrocardiographic recordings were performed for arrhythmia analysis and for the measurement of time domain indices of heart rate variability. Patients were separated into 2 groups, according to their ventricular arrhythmia density. The arrhythmia group (n = 11) included patients with >10 ventricular premature beats (VPBs) per hour (VPBs/h), and the heart rate variability group (n = 12) included patients with a number of VPBs in 24 hours not exceeding 1% of the total number of R-R intervals.

RESULTS

For the arrhythmia group, pyridostigmine resulted in a 65% reduction of ventricular ectopic activity (placebo 266 +/- 56 VPBs/h vs pyridostigmine 173 +/- 49 VPBs/h, P =.03). For the heart rate variability group, pyridostigmine administration increased mean R-R interval (placebo 733 +/- 22 ms vs pyridostigmine 790 +/- 33 ms, P =.01), and in the time domain indices of heart rate variability root-mean-square of successive differences (placebo 21 +/- 2 ms vs pyridostigmine 27 +/- 3 ms, P =.01) and percentage of pairs of adjacent R-R intervals differing by >50 ms (placebo 3% +/- 1% vs pyridostigmine 6% +/- 2%, P =.03).

CONCLUSION

In patients with heart failure, pyridostigmine reduced ventricular arrhythmia density and increased heart rate variability, most likely due to its cholinomimetic effect. Long-term trials with pyridostigmine in heart failure should be conducted.

摘要

背景

心力衰竭患者室性心律失常密度增加和心率变异性降低与死亡风险相关。溴吡斯的明抑制胆碱酯酶可增加正常受试者的心率变异性，但其对心力衰竭患者的影响尚不清楚。在本研究中，我们检验了以下假设：短期给予胆碱酯酶抑制剂溴吡斯的明可降低充血性心力衰竭患者的室性心律失常密度并增加心率变异性。

方法

心力衰竭且处于窦性心律的患者参与了一项双盲、交叉试验方案，随机接受安慰剂和吡斯的明治疗（口服30mg，每日3次，共2天）。进行24小时心电图记录以分析心律失常并测量心率变异性的时域指标。根据患者的室性心律失常密度将其分为2组。心律失常组（n = 11）包括每小时室性早搏（VPB）>10次（VPBs/h）的患者，心率变异性组（n = 12）包括24小时内室性早搏数量不超过R-R间期总数1%的患者。

结果

对于心律失常组，吡斯的明使室性异位活动减少65%（安慰剂组266±56 VPBs/h，吡斯的明组173±49 VPBs/h，P = 0.03）。对于心率变异性组，给予吡斯的明可增加平均R-R间期（安慰剂组733±22 ms，吡斯的明组790±33 ms，P = 0.01），并且在心率变异性的时域指标方面，连续差值的均方根（安慰剂组21±2 ms，吡斯的明组27±3 ms，P = 0.01）以及相邻R-R间期差值>50 ms的配对百分比（安慰剂组3%±1%，吡斯的明组6%±2%，P = 0.03）均增加。