Noda T, Minatoguchi S, Fujii K, Hori M, Ito T, Kanmatsuse K, Matsuzaki M, Miura T, Nonogi H, Tada M, Tanaka M, Fujiwara H
Second Department of Internal Medicine, Gifu University School of Medicine, Japan.
J Am Coll Cardiol. 1999 Dec;34(7):1966-74. doi: 10.1016/s0735-1097(99)00462-3.
This study aimed to investigate prospectively the protective effect of a first preinfarction angina attack against acute myocardial infarction (AMI) in human hearts without significant collaterals.
Several retrospective studies and the prospective studies have demonstrated the existence of the preconditioning (PC) effect in humans. However, collaterals were not examined in the prospective studies. In animal models, the PC effect on myocardial infarct size appears soon after PC reperfusion (classic) but disappears within 1 to 2 h. It then reappears 24 to 48 h after reperfusion (the delayed PC effect). Meanwhile, the PC effect on stunning appears 12 h after PC reperfusion (the delayed PC effect). The concept of the classic and delayed PC effects has not been investigated in human AMI studies. If the above concept is also correct in humans, the infarct size and/or impairment of the left ventricular function should be inversely correlated with the time interval between the first preinfarction angina attack and the onset of AMI when that time interval is limited to between 2 and 48 h.
The subjects were 25 patients with first AMI of the proximal left anterior descending artery who underwent successful direct percutaneous transluminal coronary angioplasty (PTCA) 2 to 6 h after the onset and with no (or poor) collateral circulation (grade 0 or 1). They were divided into two groups: preinfarction angina (PA)(+) group: 11 patients with new onset preinfarction angina from 2 to 48 h before the onset, PA(-) group: 14 patients without angina before infarction. Peak creatine kinase (CK) and cumulative CK were examined, and the left ventricular ejection fraction (LVEF) and the regional wall motion (RWM) were determined from the left ventriculograms during the acute (immediately after the coronary reperfusion) and chronic (four weeks after the onset of AMI) phases. The RWM index (RWMI) was then calculated as the mean motion of chords (standard deviation [SD]/chord) lying in the area of chords of RWM < or = -2 SD in the acute phase (ischemic risk area). RESULTS The increase in the RWMI between the acute and chronic phases was significantly larger in the PA(+) group than in the PA(-) group (1.55 +/- 1.32 and 0.69 +/- 0.75, p < 0.05, respectively) although no significant difference in the enzymatic infarct size was seen between the two groups. The increases in the LVEF and the RWMI were significantly correlated with the time interval from the first preinfarction angina attack to the onset of AMI (r = 0.622, p < 0.05 and r = 0.646, p < 0.05, respectively), but the enzymatic infarct size was not.
The beneficial effect of preinfarction angina on left ventricular wall motion, independently of collateral flows, indicates the existence of the PC effect in humans. The greater protective effect of a longer time interval between angina pectoris and AMI suggests that the protection is due to a delayed PC effect.
本研究旨在前瞻性地调查首次梗死前心绞痛发作对无明显侧支循环的人类心脏急性心肌梗死(AMI)的保护作用。
多项回顾性研究和前瞻性研究已证明人类存在预处理(PC)效应。然而,前瞻性研究中未对侧支循环进行检查。在动物模型中,PC对心肌梗死面积的影响在PC再灌注后很快出现(经典效应),但在1至2小时内消失。然后在再灌注后24至48小时再次出现(延迟PC效应)。同时,PC对心肌顿抑的影响在PC再灌注后12小时出现(延迟PC效应)。经典和延迟PC效应的概念在人类AMI研究中尚未得到研究。如果上述概念在人类中也正确,那么当梗死前心绞痛发作与AMI发作之间的时间间隔限制在2至48小时时,梗死面积和/或左心室功能损害应与该时间间隔呈负相关。
研究对象为25例左前降支近端首次发生AMI且在发病后2至6小时接受成功直接经皮腔内冠状动脉成形术(PTCA)且无(或侧支循环差)(0级或1级)的患者。他们被分为两组:梗死前心绞痛(PA)(+)组:11例在发病前2至48小时新发梗死前心绞痛的患者,PA(-)组:14例梗死前无心绞痛的患者。检测峰值肌酸激酶(CK)和累积CK,并在急性期(冠状动脉再灌注后立即)和慢性期(AMI发病后四周)从左心室造影中测定左心室射血分数(LVEF)和室壁运动(RWM)。然后计算RWM指数(RWMI),即急性期(缺血危险区)RWM≤-2标准差区域内弦的平均运动(标准差[SD]/弦)。结果:PA(+)组急性期和慢性期之间RWMI的增加显著大于PA(-)组(分别为1.55±1.32和0.69±0.75,p<0.05),尽管两组间酶学梗死面积无显著差异。LVEF和RWMI的增加与首次梗死前心绞痛发作至AMI发作的时间间隔显著相关(分别为r=0.622,p<0.05和r=0.646,p<0.05),但酶学梗死面积与时间间隔无关。
梗死前心绞痛对左心室壁运动的有益作用独立于侧支血流,表明人类存在PC效应。心绞痛与AMI之间较长时间间隔具有更大的保护作用,提示这种保护作用归因于延迟PC效应。
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