Inaba H, Numai T, Araki M, Mizuguchi T
Department of Anesthesiology, Chiba University School of Medicine, Japan.
Surg Today. 1993;23(3):234-40. doi: 10.1007/BF00309233.
To investigate whether the inhibition of protein kinases including protein kinase C can antagonize endotoxicosis, the in vivo effects of K252a, a potent inhibitor of protein kinases, on endotoxin-induced lethality and glucose dyshomeostasis were determined in conscious rats. Sprague-Dawley rats (260-340 g) were divided into the following four groups: Group DS, 2.5% dimethyl sulfoxide (DMSO), 6 ml/kg iv + 0.9% saline, 2 ml/kg iv; group KS, K252a in 2.5% DMSO, 4 mg/kg iv + 0.9% saline; group DE, 2.5% DMSO + endotoxin (E. coli), 15 mg/kg iv; and group KE, K252a in 2.5% DMSO + endotoxin. A quarter of DMSO or K252a solution was continuously infused over a 15 min period before a bolus injection of either saline or endotoxin. The remaining dose was administered over a 180 min period after saline or endotoxin. All animals in the DS and KS groups survived for 24 hrs. K252a significantly improved endotoxic lethality. It attenuated the initial hyperglycemia, and late hypoglycemia, hyperlactacidemia, and base deficit after endotoxin. However, K252a had no influence on the endotoxic alterations of blood pressure, PaCO2 or PaO2. These results suggest that the activations of protein kinases, particularly protein kinase C, are involved in the pathogenesis of lethal endotoxicosis and sepsis.
为研究包括蛋白激酶C在内的蛋白激酶抑制作用是否能拮抗内毒素血症,我们在清醒大鼠中测定了蛋白激酶强效抑制剂K252a对内毒素诱导的致死率和葡萄糖稳态失衡的体内效应。将体重260 - 340 g的Sprague-Dawley大鼠分为以下四组:DS组,2.5%二甲基亚砜(DMSO),6 ml/kg静脉注射 + 0.9%生理盐水,2 ml/kg静脉注射;KS组,2.5% DMSO中的K252a,4 mg/kg静脉注射 + 0.9%生理盐水;DE组,2.5% DMSO + 内毒素(大肠杆菌),15 mg/kg静脉注射;KE组,2.5% DMSO中的K252a + 内毒素。在推注生理盐水或内毒素前15分钟内持续输注四分之一剂量的DMSO或K252a溶液。剩余剂量在注射生理盐水或内毒素后的180分钟内给予。DS组和KS组的所有动物均存活24小时。K252a显著改善了内毒素致死率。它减轻了内毒素注射后的初始高血糖、后期低血糖、高乳酸血症和碱缺失。然而,K252a对血压、PaCO2或PaO2的内毒素性改变没有影响。这些结果表明,蛋白激酶尤其是蛋白激酶C的激活参与了致死性内毒素血症和脓毒症的发病机制。
