摘要
目的探讨缺血预处理(IPC)在肝缺血再灌注(I/R)损伤中的作用及腺苷在此过程中的作用机制.方法采用大鼠原位肝I/R模型,缺血前舌静脉注射腺苷(adenosine,100mg/kg),或硫苯茶碱(SPT,10mg/kg),观察血ALT,AST及肝组织LPO,GSHPx和SOD变化.结果IPC降低了血ALT,AST及肝组织自由基水平(ALT,nmol/s,783±200vs2801±217;AST,nmol/s,1667±333vs3134±600;LPO,μmol/g,045±011vs061±013;GSHPx,KEU/g,222±030vs156±025,P<001).施加腺苷后,血ALT,AST及肝组织自由基水平较I/R组明显下降,呈现出类似IPC的保护作用(ALT,nmol/s,1117±183vs2801±217;AST,nmol/s,2167±283vs3134±600;LPO,μmol/g,046±011vs061±013;GSHPx,KEU/g,234±035vs156±025;P<001).当施加腺苷受体的阻滞剂SPT后,IPC的保护作用被消除(A?
AIM
To investigate the effects of ischemic preconditioning (IPC) on hepatic ischemia/ reperfusion (I/
R) in vivo , as well as the implication of adenosine in this process. METHODS The rat model
of in situ hepatic I/ R injury was intravenously injected with adenosine (100 mg/ kg) or 8 p
sulfophenyl theophylline (10 mg/ kg) before hepatic ischemia and reperfusion. RESULTS IPC
prevented the increases in serum ALT, AST activities and level of hepatic oxygen free radicals
(ALT, nmol/ s , 783±200 vs 2801±217; AST, nmol/ s , 1667±333 vs 3134±600; LPO,
μmol/ g , 0 45±0 11 vs 0 61±0 13; GSH Px, KEU/ g , 2 22±0 30 vs 1 56±0 25,
P <0 01). Pretreatment with adenosine simulated the effect of IPC (ALT, nmol/ s , 1117±183
vs 2801±217; AST, nmol/ s , 2167±283 vs 3134±600; LPO, μmol/ g , 0 46±0 11
vs 0 61±0 13;GSH Px, KEU/ g , 2 34±0 35 vs 1 56±0 25; P <0 01). However,
inhibition of adenosine abolished the protective effect (ALT, nmol/ s , 2501±250 vs 2801±
217; AST, nmol/ s , 3084±583 vs 3134±600; LPO, μmol/ g , 0 59±0 13 vs 0 61±
0 13;GSH Px, KEU/ g , 1 59±0 24 vs 1 56±0 25; P >0 05). CONCLUSION Adenosine
plays a protective role in hepatic IPC and its mechanism may be inactivated oxygen free
radicals.
出处
《世界华人消化杂志》
CAS
1999年第4期298-299,共2页
World Chinese Journal of Digestology
关键词
肝缺血
腺苷
预处理
再灌注损伤
hepatic ischemia
adenosine
8 p sulfophenyl theophylline
