摘要
目的探讨心肌缺血预处理(myocardial ischemic preconditioning,MIP)对缺血-再灌注(Ischemia/Reperfusion,I/R)期血小板活化、血管内血栓形成的影响。方法40只成年新西兰大白兔随机分为缺血-再灌注对照组和缺血预处理(ischemic precondi-tioning,IPC)组(n=20),分别在基础状态、缺血前、缺血40min、再灌注60min和再灌注120min测定血浆可溶性P-选择素(sP-selectin)、血栓烷B2(TXB2)的浓度(n=12)。另一方案则通过颈总动脉—颈外静脉旁路法观测基础状态和再灌注60min时的血栓湿重(n=8)。结果再灌注期,两组实验动物sP-selectin、TXB2浓度和血栓湿重与基础状态时相比均升高(P<0.05);组间比较,IPC组上述参数均低于对照组,再灌注60min和120min时差异均有显著性。结论心肌缺血预处理可以有效抑止再灌注期血小板活化、限制血管内血栓形成。
Objective To evaluate the effects of myocardium ischemic preconditioning in inhibiting platelet activation and thrombus for marion during ischemia reperfusion.Methods Forty new Zealand white rabbits were divided into control group (Ischemia/Reperfusion I/R ) and ischemic preconditioning group(IPC) (n=20)randomly. Soluble P-selectin (sP-selectin)and thromboxane B2 (TXB2)were measured at baseline,pre-occlusion,occlusion 40 minutes, reperfusion 60minutes and reperfusion 120minutes respectively(n=12). Thrombus were formed through Carotid- jugular vein bypass and weighted at baseline and reperfusion 60minutes (n=8). Results During ischemia-reperfusion periods,compared with control subjects, IPC rabbits had:(1)lower sP-selectin and TXB2 plasma concentrations at reperfusion 60 minutes and reperfusion 120minutes (both P〈0.05);(2) less thrombus weight at reperfusion 60minutes (P〈0.05). Con, clusion IPC can inhibit platelet activation and limit thrombus growth during the ischemia-reperfusion period.
出处
《江西医药》
CAS
2007年第3期205-208,共4页
Jiangxi Medical Journal
关键词
心肌
缺血预处理
血小板
血拴
myocardium
ischemic preconditioning
platelet
thrombus
