脑缺血Akt和MAPK磷酸酶负性调节c-Jun N端激酶信号通路  被引量:1

Relationship Between Akt and MAPK Phosphatase and Activity of c-Jun N-terminal Kinase in Rats after Cerebral Ischemia Reperfusion

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作  者:朱建熹[1] 沈术彤[2] 高丽[3,4] 沈伟[3,4] 郭军[1,2] 

机构地区:[1]南京医科大学生物化学和分子生物学系,江苏南京210029 [2]南京医科大学基础医学中心实验室,江苏南京210029 [3]南京医科大学南京脑科医院 [4]南京医科大学神经内科,江苏南京210029

出  处:《现代生物医学进展》2011年第11期2018-2021,共4页Progress in Modern Biomedicine

基  金:国家自然科学基金(30871200);南京医科大学科技发展基金重点项目(08NMUZ006)

摘  要:目的:探讨脑缺血再灌后Akt和MAPK磷酸酶与JNK活性下调的关系。方法:采用成年清洁级雄性SD大鼠,建立四动脉阻断前脑缺血再灌注模型。缺血10min后再灌注不同时间(15min,1h,4h,24h)。侧脑室分别给予PI3K抑制剂LY294002(LY)和MAPK磷酸酶抑制剂放线菌酮(CHO)。免疫印迹观察p-Akt和p-JNK蛋白水平变化。结果:脑缺血再灌注4h,JNK的活性能被Akt抑制剂LY294002增强,表明激活的Akt能够下调JNK信号通路。而MAPK磷酸酶抑制剂放线菌酮能上调缺血后JNK活性,提示MAPK磷酸酶通过去磷酸化参与了JNK的活性抑制。结论:前脑缺血再灌后,激活Akt和MAPK磷酸酶参与了JNK信号通路负性调节,是抑制JNK诱导缺血后中枢神经损伤的重要机制。Objective: To investigate the relationship between the of c-Jun N-terminal kinase (JNK) pathway and Akt and MKP Methods: Rats in the experimental group were subjected to four-vessel occlusion method, endured 10 min ischemia followed by reperfusion for 15min, lh, 4h and 24h to examine phosphorylation of JNK and its upstream Akt in the rat hippocampi. The PI3K inhibitor LY294002 and MAPK phosphatase inhibitor cycloheximide were administrated to the rat hippocampi to observe the change of JNK activity. Results: JNK activity at 4h was enhanced obviously, which suggested that activated Akt suppresses the JNK pathway. Moreover, the JNK activity at 4h was also largely enhanced by cycloheximide, which indicated that the inactivation of JNK by phosphatases occurs at about 4 h via its dephosphorylation. Conclusion: Both Akt and MAPK phosphatase negatively regulate JNK pathway during cerebral ischemia in rat hippocampi.

关 键 词:前脑缺血 JNK AKT MKP 

分 类 号:Q953[生物学—动物学] R743[医药卫生—神经病学与精神病学]

 

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