Genistein and tyrphostin AG 556 block the action potential shortening in septic shock.

Chern-En Chiang, Hsiang-Ning Luk, Tsui-Min Wang, Joen-Rong Sheu, Philip Yu-An Ding
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Abstract

Background: We have previously shown that an increase in NO activity activated ATP-sensitive potassium channel (K(ATP)) and shortened action potential duration (APD) in an endotoxic shock model. Because the increase in NO production and the decrease of APD appear to be downstream late events in endotoxic shock, we hypothesized that a common signaling pathway might mediate these effects.

Methods: Using a guinea pig model of endotoxic shock, we investigated the effect of genistein and tyrphostin AG 556 on the cardiac action potential. Adult Hartley guinea pigs (300 to 450 gm) were randomized into 2 treatment parts. In the chronic treatment part, guinea pigs were randomized to receive daily subcutaneous injection of one of the five agents: saline, genistein, tyrphostin AG 556, daidzein, and vehicle for 10 days. In the acute treatment part, these agents were administered by intraperitoneal injection 1 hour before endotoxic shock. The animals were then anesthetized and mechanically ventilated, and underwent 6-hour endotoxic shock or sham experiment.

Results: In the chronic treatment part, the plasma nitrate concentration, myocardial guanosine 3',5'-cyclic monophosphate (cGMP) content, and APD at 90% repolarization (APD90) of papillary muscle showed no difference in the five groups before endotoxic shock. After 6-hour endotoxic shock, the elevation of plasma nitrate concentration and myocardial cGMP content was found significant in the control, the daidzein, and the vehicle groups, but was blunted in the genistein and the tyrphostin groups. The shortening of APD90 of papillary muscle was also significant in the control, the daidzein, and the vehicle groups, but blunted in the genistein and tyrphostin groups. There were similar findings in the acute treatment part, except the weaker effect of genistein and tyrphostin.

Conclusions: Genistein and tyrphostin AG 556, either administered chronically or acutely, significantly attenuate the cardiac APD shortening in endotoxic shock, presumably through the decrease in the plasma nitrate and the cardiac cGMP production. It is suggested that tyrosine kinase signaling plays an important role in the modulation of APD in endotoxic shock.

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染料木素和tyrphostin AG 556阻断败血性休克的动作电位缩短。
背景:我们之前已经表明,在内毒素休克模型中,NO活性的增加激活了ATP敏感的钾通道(K(ATP))并缩短了动作电位持续时间(APD)。由于一氧化氮生成的增加和APD的减少似乎是内源性休克的下游晚期事件,我们假设一个共同的信号通路可能介导这些作用。方法:采用内源性休克豚鼠模型,观察染料木素和tyrphostin AG 556对心脏动作电位的影响。成年哈特利豚鼠(300 ~ 450 gm)随机分为2个处理组。在慢性治疗部分,豚鼠随机接受每日皮下注射生理盐水、染料木素、tyrphostin AG 556、大豆苷元和载药中的一种,持续10天。在急性治疗部分,这些药物在内源性休克前1小时腹腔注射。麻醉、机械通气后,进行6小时内毒素休克或假实验。结果:慢性治疗部分,内毒素休克前5组大鼠血浆硝酸盐浓度、心肌鸟苷3′,5′-环单磷酸(cGMP)含量、乳头肌90%复极APD (APD90)无显著差异。内源性休克6小时后,血浆硝酸盐浓度和心肌cGMP含量在对照组、大豆苷元组和载药组均有显著升高,而染料木素组和tyrphostin组均无明显升高。对照组、大豆苷元组和载药组大鼠乳头肌APD90缩短明显,染料木素组和tyrphostin组大鼠乳头肌APD90缩短明显。在急性治疗部分,除染料木素和tyrphostin的作用较弱外,结果相似。结论:染料木素和tyrphostin AG 556慢性或急性给药可显著减轻内源性休克时心脏APD缩短,可能是通过降低血浆硝酸盐和心脏cGMP的产生。提示酪氨酸激酶信号在内毒素休克APD的调控中起重要作用。
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