Lalu Manoj M, Gao Cindy Q, Schulz Richard
Department of Pharmacology, Cardiovascular Research Group, University of Alberta, Edmonton, Alberta, Canada.
Mol Cell Biochem. 2003 Sep;251(1-2):61-6.
Enhanced cardiac generation of peroxynitrite contributes to septic cardiomyopathy. Since matrix metalloproteinases (MMPs) are activated in vitro by peroxynitrite, we hypothezised that MMPs may contribute to cardiac mechanical dysfunction in sepsis. Rats were injected (i.p.) with either lipopolysaccharide (LPS, 4 mg/kg) or vehicle. MMP inhibitors, either Ro 31-9790 (20 mg/kg), doxycycline (4 mg/kg), or vehicle were administered i.p. 30 min after LPS. At 6 h, when the symptoms of endotoxemia peak, hearts were excised and perfused as working hearts with Krebs-Henseleit buffer at 37 degrees C. Cardiac work (cardiac output x peak systolic pressure product) was measured. Perfusate and ventricle samples were analyzed by gelatin zymography to quantify MMP activity. Cardiac function was significantly depressed in LPS-treated rats compared to control rats (control: 55 +/- 4, LPS: 26 +/- 6 mmHgmLmin(-1)). LPS also caused a loss of 72 kDa MMP-2 activity in the ventricles and the perfusate. Although MMP-9 activity was not detected in the ventricles, LPS resulted in an increase in perfusate 92 kDa MMP-9 activity. The MMP inhibitors significantly improved cardiac function of LPS-treated rats (Ro 31-9790: 38 +/- 3, doxycycline: 51 +/- 3 mmHgmLmin(-1)), had no effect on the loss of MMP-2 activity, and significantly reduced the MMP-9 activity in the perfusate. These results demonstrate, for the first time, that LPS induced cardiac dysfunction is associated with a loss in ventricular MMP-2 activity and the release of MMP-9 from the heart. MMP inhibitors can significantly preserve cardiac mechanical function during septic shock.
过氧亚硝酸盐在心脏中的生成增强会导致脓毒症性心肌病。由于基质金属蛋白酶(MMPs)在体外可被过氧亚硝酸盐激活,我们推测MMPs可能参与脓毒症时心脏的机械功能障碍。给大鼠腹腔注射脂多糖(LPS,4 mg/kg)或赋形剂。在注射LPS 30分钟后腹腔注射MMP抑制剂,分别为Ro 31-9790(20 mg/kg)、强力霉素(4 mg/kg)或赋形剂。6小时后,即内毒素血症症状达到峰值时,取出心脏并在37℃下用Krebs-Henseleit缓冲液作为工作心脏进行灌注。测量心脏做功(心输出量×收缩压峰值乘积)。通过明胶酶谱法分析灌注液和心室样本以量化MMP活性。与对照大鼠相比,LPS处理的大鼠心脏功能明显降低(对照:55±4,LPS:26±6 mmHg·mL·min⁻¹)。LPS还导致心室和灌注液中72 kDa MMP-²活性丧失。尽管在心室中未检测到MMP-9活性,但LPS导致灌注液中92 kDa MMP-9活性增加。MMP抑制剂显著改善了LPS处理大鼠的心脏功能(Ro 31-9790:38±3,强力霉素:51±3 mmHg·mL·min⁻¹),对MMP-²活性丧失无影响,并显著降低了灌注液中MMP-9活性。这些结果首次表明,LPS诱导的心脏功能障碍与心室MMP-²活性丧失和心脏释放MMP-9有关。MMP抑制剂可在脓毒症休克期间显著维持心脏机械功能。
