Department of Anaesthesia and Critical Care, University of Wuerzburg, Oberduerrbacher Str. 6, 97080 Wuerzburg, Germany.
Br J Anaesth. 2012 Apr;108(4):594-601. doi: 10.1093/bja/aer496. Epub 2012 Feb 6.
Desflurane (DES)-induced preconditioning is mediated by large-conductance calcium-activated potassium channels (BK(Ca)). Whether BK(Ca) are involved in anaesthetic-induced post-conditioning is unknown. We tested the hypothesis that DES-induced post-conditioning is mediated by BK(Ca) upstream of the mitochondrial permeability transition pore (mPTP).
Pentobarbital-anaesthetized male C57Black/6 mice were subjected to 45 min coronary artery occlusion (CAO) and 3 h reperfusion. Animals received either no intervention or dimethylsulphoxide (DMSO, 10 µl g(-1)). DES (1.0 MAC, 7.5 vol%) was administered for 18 min, starting 3 min before the end of CAO. The following agents were given either alone or in combination with DES: the BK(Ca) activator NS1619 (1 µg g(-1)), the BK(Ca) inhibitor iberiotoxin (IbTx, 0.05 µg g(-1)), the mPTP opener atractyloside (ATRA, 25 µg g(-1)), and the mPTP inhibitor cyclosporine A (CYC A, 10 µg g(-1)). Infarct size (IS) was determined with triphenyltetrazolium chloride and the area at risk with Evans Blue, respectively.
IS in control animals was 48(6)%. Neither DMSO, IbTx nor ATRA affected myocardial IS. DES alone or NS1619 alone or the combination reduced IS (P<0.05), CYC A alone or in combination with IbTx or DES also reduced IS (P<0.05). DES-induced reduction of myocardial IS was completely abolished by IbTx and was partially blocked by ATRA and ATRA partially blocked IS reduction by NS1619.
These data suggest that DES-induced post-conditioning against myocardial infarction is mediated by BK(Ca) and mPTP. Cardioprotection by BK(Ca) activator NS1619 might occur, at least in part, independently of mPTP.
地氟烷(DES)诱导的预处理是通过大电导钙激活钾通道(BK(Ca))介导的。BK(Ca)是否参与麻醉诱导的后处理尚不清楚。我们检验了这样一个假设,即 DES 诱导的后处理是通过线粒体通透性转换孔(mPTP)上游的 BK(Ca)介导的。
戊巴比妥钠麻醉的雄性 C57Black/6 小鼠接受 45 分钟的冠状动脉闭塞(CAO)和 3 小时再灌注。动物接受以下干预或不接受干预:二甲基亚砜(DMSO,10μl g(-1))。DES(1.0 MAC,7.5 体积%)在 CAO 结束前 3 分钟开始给药 18 分钟。以下试剂单独或与 DES 联合使用:BK(Ca)激活剂 NS1619(1μg g(-1)),BK(Ca)抑制剂 Iberiotoxin(IbTx,0.05μg g(-1)),mPTP opener 长春质碱(ATRA,25μg g(-1))和 mPTP 抑制剂环孢菌素 A(CYC A,10μg g(-1))。分别用三苯基四唑氯化物和 Evans Blue 测定梗死面积(IS)和危险区面积。
对照组动物的 IS 为 48(6)%。DMSO、IbTx 或 ATRA 均不影响心肌 IS。DES 单独或 NS1619 单独或联合使用均可降低 IS(P<0.05),CYC A 单独或联合使用 IbTx 或 DES 也可降低 IS(P<0.05)。IbTx 完全阻断了 DES 诱导的心肌 IS 减少,ATRA 部分阻断了 NS1619 诱导的 IS 减少,而 ATRA 部分阻断了 IS 减少。
这些数据表明,DES 诱导的心肌梗死后处理是通过 BK(Ca)和 mPTP 介导的。BK(Ca)激活剂 NS1619 介导的心脏保护作用至少部分独立于 mPTP。
