中国急救医学
中國急救醫學
중국급구의학
CHINESE JOURNAL OF CRITICAL CARE MEDICINE
2014年
8期
739-742
,共4页
苏丹颖%马晶%孙亮%张丽%王永贵
囌丹穎%馬晶%孫亮%張麗%王永貴
소단영%마정%손량%장려%왕영귀
UCF-101%脑缺血再灌注%脑保护%p38 MAPK%磷酸化水平
UCF-101%腦缺血再灌註%腦保護%p38 MAPK%燐痠化水平
UCF-101%뇌결혈재관주%뇌보호%p38 MAPK%린산화수평
UCF-101%Cerebral ischemia-reperfusion%Neuroprotection%p38 MAPK%Phosphorylation
目的:探讨UCF-101在大鼠脑缺血再灌注损伤中的作用及分子机制。方法采用线栓法建立Wistar大鼠大脑中动脉闭塞( middle cerebral arteryocclusion , MCAO)模型,随机分为假手术组、缺血再灌注组和UCF-101组,术后观察神经功能缺损症状,TUNEL法检测神经元凋亡,免疫组化法及 Western blot 检测脑皮层神经元磷酸化 p38丝裂原活化蛋白激酶( mitogen activated protein kinase , MAPK)蛋白的表达。结果 UCF-101改善大鼠脑缺血再灌注后的神经功能缺损症状,减少细胞凋亡(P<0.05);与假手术组比较,大鼠缺血后磷酸化p38 MAPK表达水平增加;与脑缺血组比较,UCF-101组磷酸化p38 MAPK表达水平有所降低( P<0.05)。结论UCF-101对脑缺血再灌注损伤有保护作用,其机制可能与p38 MAPK信号通路有关。
目的:探討UCF-101在大鼠腦缺血再灌註損傷中的作用及分子機製。方法採用線栓法建立Wistar大鼠大腦中動脈閉塞( middle cerebral arteryocclusion , MCAO)模型,隨機分為假手術組、缺血再灌註組和UCF-101組,術後觀察神經功能缺損癥狀,TUNEL法檢測神經元凋亡,免疫組化法及 Western blot 檢測腦皮層神經元燐痠化 p38絲裂原活化蛋白激酶( mitogen activated protein kinase , MAPK)蛋白的錶達。結果 UCF-101改善大鼠腦缺血再灌註後的神經功能缺損癥狀,減少細胞凋亡(P<0.05);與假手術組比較,大鼠缺血後燐痠化p38 MAPK錶達水平增加;與腦缺血組比較,UCF-101組燐痠化p38 MAPK錶達水平有所降低( P<0.05)。結論UCF-101對腦缺血再灌註損傷有保護作用,其機製可能與p38 MAPK信號通路有關。
목적:탐토UCF-101재대서뇌결혈재관주손상중적작용급분자궤제。방법채용선전법건립Wistar대서대뇌중동맥폐새( middle cerebral arteryocclusion , MCAO)모형,수궤분위가수술조、결혈재관주조화UCF-101조,술후관찰신경공능결손증상,TUNEL법검측신경원조망,면역조화법급 Western blot 검측뇌피층신경원린산화 p38사렬원활화단백격매( mitogen activated protein kinase , MAPK)단백적표체。결과 UCF-101개선대서뇌결혈재관주후적신경공능결손증상,감소세포조망(P<0.05);여가수술조비교,대서결혈후린산화p38 MAPK표체수평증가;여뇌결혈조비교,UCF-101조린산화p38 MAPK표체수평유소강저( P<0.05)。결론UCF-101대뇌결혈재관주손상유보호작용,기궤제가능여p38 MAPK신호통로유관。
Objective To investigate the neuroprotective effect and mechanisms of 5 -[5-(2-nitrophenyl)furfuryliodine]-1,3-diphenyl-2-thiobarbituric acid (UCF-101) on the cerebral neurons of rats during cerebral ischemia -reperfusion.Methods The focal cerebral ischemia models of Wistar rats were established by the middle cerebral artery occlusion ( MCAO ) with thread occlusion methods .Rats were randomly divided into sham operated group , ischemia -reperfusion group and UCF-101 treated group .24 h after focal cerebral ischemia -reperfusion , the rats were evaluated for neurological deficits and TUNEL method was used to measure apoptotic neurons , and the expression levels of p38 MAPK phosphorylation were detected by immunohistochemistry and Western blot analysis . Results UCF -101 treatment significantly improved neurological behavior and reduced TUNEL -positive cells in the cerebral cortex . Furthermore , the phosphorylation levels of p 38 MAPK were increased in ischemia-reperfusion group thanthose in sham operated group (P<0.05).In UCF-101 treated group the phosphorylation levels of p 38 MAPK was decreased compared with the ischemia -reperfusion group ( P <0 .05 ) . Conclusion p38 MAPK signal pathway might be involved in neuroprotective effect of UCF -101 treatment on focal ischemic brain of mice .
