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高、低剂量极化液对缺血/ 再灌注心肌细胞凋亡及相关基因的影响(PDF)

《心脏杂志》[ISSN:1009-7236/CN:61-1268/R]

期数:
2004年第5期
页码:
427-430
栏目:
基础研究
出版日期:
2004-09-01

文章信息/Info

Title:
Comparative study of the effects of high dose and low dose GIK on cardiomyocyte apoptosis and apoptosis related genes during myocardial ischemic and reperfusion
作者:
高 晖1张 清1贾国良1张荣庆1马兰香2赵新国2王 岚2
1. 第四军医大学西京医院心血管内科, 陕西西安710032 ; 2.武警陕西总队医院心血管内科,陕西西安710054
Author(s):
GAO Hui1ZHANG Qing1JIA Guo-liang1ZHANG Rong-qing1MA Lan-xiang2ZHAO Xin-guo2WANG Lan2
11Department of Cardiology , Xijing Hospital , Fourth Military Medical University , Xi’an , Shaanxi 710032 , China; 21Department of Cardiology , Shaanxi Provincial Corps Hospital , Chinese People’s Armed Police Forceds , Xi’an , Shaanxi 710054 , China
关键词:
胰岛素 再灌注损伤 心肌缺血 细胞凋亡 超微结构
Keywords:
insulin Myocardial ischemia reperfusion apoptosis ultrastructure
分类号:
R542. 2
DOI:
-
文献标识码:
A
摘要:
目的: 探讨高、低两种剂量葡萄糖- 胰岛素- 钾极化液(GIK) 对缺血/ 再灌注(MI/ R) 心肌超微结构,细胞凋亡 及其相关基因的影响。方法: 制备兔MI/ R 模型,分别用生理盐水,低剂量极化液(LGIK) ,高剂量极化液(HGIK) 干 预分组。检验心肌组织SOD 活性,原位末端标记(TUNEL) 法测定凋亡心肌细胞,免疫组化SP 法测定Bcl-2 , Fas 的 含量,在电镜下观察心肌细胞的超微结构。结果:与对照组比较,HGIK组SOD 活性增加( P < 0. 01) ,凋亡指数(AI) 和Fas 含量减少( P < 0. 01) , Bcl-2 含量增加( P < 0. 01) 。心肌细胞超微结构表现为损伤减轻。LGIK亦可增加SOD 活性和Bcl-2 含量( P < 0. 05) ,减少AI 和Fas( P < 0. 05) 含量。结论: GIK具有抗缺血/ 再灌注损伤的作用,其机制可 能是通过调节Bcl-2 和Fas 介导的心肌缺血/ 再灌注细胞凋亡而实现。高剂量GIK对缺血/ 再灌注心肌细胞的保护 作用显著大于低剂量GIK( P < 0. 05) 。
Abstract:
AIM: To study the effect of different doses of glucose-insulin-potassium (GIK) cocktail on cardiac myocyte apoptosis and ultrastructure following myocardial ischemia/ reperfusion (MI/ R) . METHODS: Rabbits were subjected to 45 min myocardial ischemia , followed by reperfusion for 3 h. Anesthetized rabbits were randomly treated with continuous infusion of saline , LGIK (100 g/ L Glucose ,20 U/ L Insulin and 20 mmol/ L KCl) , HGIK (300 g/ L Glucose , 50 U/ L Insulin and 80 mmol/ L KCl) , 5 min before the reperfusion and throughout the 3 h reperfusion. The animals were sacrificed and the heart was harvested for SOD and ultrastructure examination(electron microscope) . Apoptosis was identified by TUNEL and apoptosis index (AI)was obtained. The expressions of Fas ,Bcl-2 protein were measured by immunohistochemical technique. SOD was assayed spectrophocometrically and myocardial ultrastructure was examined. RESULTS : Compared with the vehicle treated rabbits , the HGIK-treated rabbits showed protection against MI/ R injury as evidenced by marked decrease of AI and the content of Fas protein ( P < 0. 01) , significantly increased the content of Bcl-2 protein and activity of SOD( P < 0. 01) . The ultrastructure of myocardium showed attenuated injury. AI and the content of Fas protein of the LGIK-treated rabbits were reduced ( P < 0. 05) , and the content of Bcl-2 protein and activity of SOD were improved( P < 0. 05) . CONCLUSION: GIKcan protect myocardiumfrom MI/ R injury by modulating the expressions of Fas and Bcl22 protein and inhibit apoptosis following myocardial MI/R and the high dose of GIKplay a more important role in protecting myocardial ischemia reperfusion than that of the low dose of GIK.

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备注/Memo

备注/Memo:
收稿日期:2003-8-1
更新日期/Last Update: 2004-09-01