新型心脏选择性ATP敏感性钾通道拮抗剂1-[[5-[2-(5-氯-邻茴香酰胺基)乙基]-β-甲氧基乙氧基苯基]磺酰基]-3-甲基硫脲钠盐(HMR 1402)对心肌缺血诱导的心室颤动易感性的影响:体外和体内研究
Effects of a novel cardioselective ATP-sensitive potassium channel antagonist, 1-[[5-[2-(5-chloro-o-anisamido)ethyl]-beta-methoxyethoxyphenyl]sulfonyl]-3-methylthiourea, sodium salt (HMR 1402), on susceptibility to ventricular fibrillation induced by myocardial ischemia: in vitro and in vivo studies.
作者信息
Billman George E, Houle Melanie S, Englert Heinrich C, Gögelein Heinz
机构信息
Department of Physiology and Cell Biology, The Ohio State University, 304 Hamilton Hall, 1645 Neil Avenue, Columbus, OH 43210-1218, USA.
出版信息
J Pharmacol Exp Ther. 2004 Apr;309(1):182-92. doi: 10.1124/jpet.103.061416. Epub 2004 Jan 13.
In the present study, a novel sulfonylthiourea, 1-[[5-[2-(5-chloro-o-anisamido)ethyl]-beta-methoxyethoxyphenyl]sulfonyl]-3-methylthiourea, sodium salt (HMR 1402), was investigated using in vitro and in vivo systems. HMR 1402 inhibited rilmakalim-induced currents in rat and guinea pig myocytes (IC(50) = 60 and 509 nM, respectively). Hypoxia-induced shortening of action potential duration at 90% repolarization was also significantly attenuated by HMR 1402 (68.1 +/- 3.9% of control at 0.3 microM). In contrast, HMR 1402 had a smaller effect on pancreatic beta-cells (rat insuloma cells, RINm5F) hyperpolarized with 100 microM diazoxide (IC(50) = 3.9 microM, compared with glibenclamide IC(50) = 9 nM). In a similar manner, hypoxia induced increases in coronary flow in isolated guinea pig hearts were only slightly reduced by HMR 1402. These data strongly suggest that HMR 1402 has pharmacological selectivity for cardiac myocytes and, therefore, may protect against ischemically induced ventricular fibrillation (VF) without the untoward effects of nonselective compounds. To test this hypothesis, VF was induced in 8 dogs with healed myocardial infarctions by a 2-min coronary occlusion during the last minute of exercise. On a subsequent day, the exercise plus ischemia test was repeated after HMR 1402 (3.0 mg/kg i.v., n = 4, infusion 4 microg/kg/min for 1 h before exercise, n = 4). This drug significantly reduced the incidence of VF protecting seven of eight animals (p = 0.0007) without altering plasma insulin, blood glucose, or the increases in mean coronary blood flow induced by either exercise or 15-s coronary occlusions. Thus, the ATP-sensitive potassium channel antagonist HMR 1402 can prevent ischemically induced VF without altering coronary blood flow or blood glucose.
在本研究中,使用体外和体内系统对一种新型磺酰基硫脲,即1-[[5-[2-(5-氯-邻茴香酰胺基)乙基]-β-甲氧基乙氧基苯基]磺酰基]-3-甲基硫脲钠盐(HMR 1402)进行了研究。HMR 1402抑制大鼠和豚鼠心肌细胞中瑞马卡林诱导的电流(IC(50)分别为60和509 nM)。HMR 1402也显著减弱了缺氧诱导的动作电位时程在90%复极化时的缩短(在0.3 μM时为对照的68.1±3.9%)。相比之下,HMR 1402对用100 μM二氮嗪超极化的胰腺β细胞(大鼠胰岛细胞瘤细胞,RINm5F)的作用较小(IC(50) = 3.9 μM,而格列本脲的IC(50) = 9 nM)。以类似的方式,HMR 1402仅轻微降低了缺氧诱导的离体豚鼠心脏冠状动脉血流量的增加。这些数据强烈表明,HMR 1402对心肌细胞具有药理学选择性,因此,可能预防缺血诱导的心室颤动(VF),而不会产生非选择性化合物的不良影响。为了验证这一假设,在8只心肌梗死已愈合的犬中,在运动的最后一分钟通过2分钟冠状动脉闭塞诱导VF。在随后的一天,在给予HMR 1402(3.0 mg/kg静脉注射,n = 4,在运动前1小时以4 μg/kg/分钟的速度输注,n = 4)后重复运动加缺血试验。该药物显著降低了VF的发生率,保护了8只动物中的7只(p = 0.0007),而不改变血浆胰岛素、血糖或运动或15秒冠状动脉闭塞诱导的平均冠状动脉血流量的增加。因此,ATP敏感性钾通道拮抗剂HMR 1402可以预防缺血诱导的VF,而不改变冠状动脉血流量或血糖。
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