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中年大鼠心脏缺血耐受性的变化及缺血预处理的作用

Changes in ischemic tolerance and effects of ischemic preconditioning in middle-aged rat hearts.

作者信息

Tani M, Suganuma Y, Hasegawa H, Shinmura K, Hayashi Y, Guo X, Nakamura Y

机构信息

Department of Geriatric Medicine, Keio University School of Medicine, Tokyo, Japan.

出版信息

Circulation. 1997 Jun 3;95(11):2559-66. doi: 10.1161/01.cir.95.11.2559.

DOI:10.1161/01.cir.95.11.2559
PMID:9184587
Abstract

BACKGROUND

Although both clinical and animal studies have shown that ischemic tolerance is reduced in the senescent myocardium, it has not been clarified when myocardium becomes more vulnerable to ischemia. Preconditioning protects the hearts of young adult animals of various species, but its effects are not identical in human studies. We investigated whether ischemic tolerance and the effect of preconditioning decreased in isolated hearts of middle-aged rats.

METHODS AND RESULTS

The hearts of young adult rats (12 weeks old: group Y, n = 44) and middle-aged rats (50 weeks old: group M, n = 44) were subjected to global ischemia for 15, 20, or 25 minutes followed by reperfusion. Hearts were also subjected to preconditioning and then to 20 (group Y, n = 22) or 15 (group M, n = 22) minutes of ischemia followed by reperfusion. Left ventricular developed pressure (LVDP) was decreased by 40% to 60%, and the level of ATP was decreased by 60% to 70% in group M compared with group Y. Preconditioning increased LVDP (% LVDP, 40.5% to 72.4%) and levels of high-energy phosphates (ATP, 11.8 to 14.1; creatine phosphate, 17.0 to 23.1 mumol/g dry wt) and reduced left ventricular end-diastolic pressure (LVEDP, 32.8 to 10.3 mm Hg), creatine kinase release (257 to 132 U/g dry wt), and ryanodine-sensitive sarcoplasmic reticulum Ca2+ release after ischemia in group Y. Preconditioning exerted opposite effects in group M (% LVDP, 45.9% to 15.8%; LVEDP, 21.0 to 28.5 mm Hg; ATP, 14.1 to 8.5 mumol/g dry wt; and CK release, 176 to 332 U/g dry wt). Preconditioning was associated with increases in the incidence of reperfusion-induced ventricular fibrillation (0% to 62.5%) and the rate of sarcoplasmic reticulum Ca2+ release in group M.

CONCLUSIONS

These results indicate that hearts became more vulnerable to ischemia with age and that the beneficial effects of preconditioning were reversed in middle-aged rat hearts.

摘要

背景

尽管临床和动物研究均表明衰老心肌的缺血耐受性降低,但心肌何时变得更易受缺血影响尚未明确。预处理可保护多种成年幼龄动物的心脏,但在人体研究中其效果并不相同。我们研究了中年大鼠离体心脏的缺血耐受性及预处理效果是否降低。

方法与结果

成年幼龄大鼠(12周龄:Y组,n = 44)和中年大鼠(50周龄:M组,n = 44)的心脏分别进行15、20或25分钟的全心缺血,随后再灌注。心脏也先进行预处理,然后分别进行20分钟(Y组,n = 22)或15分钟(M组,n = 22)的缺血,随后再灌注。与Y组相比,M组左心室舒张末压(LVDP)降低40%至60%,ATP水平降低60%至70%。预处理可提高Y组的LVDP(LVDP%,40.5%至72.4%)和高能磷酸盐水平(ATP,11.8至14.1;磷酸肌酸,17.0至23.1μmol/g干重),并降低左心室舒张末压(LVEDP,32.8至10.3 mmHg)、肌酸激酶释放(257至132 U/g干重)以及缺血后兰尼碱敏感的肌浆网Ca2+释放。预处理在M组产生相反的效果(LVDP%,45.9%至15.8%;LVEDP,21.0至28.5 mmHg;ATP,14.1至8.5μmol/g干重;CK释放,176至332 U/g干重)。预处理与M组再灌注诱导的室颤发生率增加(0%至62.5%)以及肌浆网Ca2+释放速率增加有关。

结论

这些结果表明,心脏随着年龄增长对缺血更敏感,且预处理的有益作用在中年大鼠心脏中发生了逆转。

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