摘要
目的研究JAK2/STAT3信号通路在河豚毒素(tetrodotoxin,TTX)心脏停搏液心肌保护中的作用。方法 24只Wistar大鼠随机均分为对照组、TTX组和TTX+AG 490组,每组8只。对照组:开胸取左心室肌作为缺血前对照。TTX组:建立离体心脏Langendorff-Neely灌注模型,预灌注K-H缓冲液30min后,灌注4℃TTX心脏停搏液,停搏心脏并低温维持60min,复灌K-H缓冲液60min后,取左心室肌备用。TTX+AG490组:操作同TTX组,但预灌和复灌时均在K-H缓冲液中加入JAK2抑制剂AG490(5μmol/L)。采用免疫组化法测定心肌组织中p-STAT3(磷酸化STAT3)和HSP 70表达量(protein expression index,PEI),TUNEL检测心肌细胞凋亡指数(apoptosis index,AI),比较组间的变化。结果与对照组相比,TTX组和TTX+AG490组心肌组织中p-STAT3和HSP 70的表达量均明显增加(P<0.05);予以AG490处理后,p-STAT3和HSP 70的表达量较TTX组明显下降(P<0.05)。HSP 70蛋白表达与p-STAT3蛋白表达呈正相关(r=0.826,P<0.05)。经历缺血再灌注后,TTX组和TTX+AG490组心肌细胞AI明显高于对照组(P<0.05);与TTX组相比,TTX+AG490组AI显著增加(P<0.05)。结论 JAK2/STAT3信号通路通过上调HSP 70的表达,调动心脏内源性保护机制,介导TTX心脏停搏液对缺血心肌的保护作用。
Objective To investigate the effect of JAK2/STAT3 pathway on myocardial protection of tetrodotoxin(TTX) cardioplegia in rat hearts.Methods 24 Wistar rats were randomly divided into Group Conteeerol,Group TTX and Group TTX+AG490(n=8).The left ventricular samples in Group Control were collected as pre-ischemia control through thoracotomy.After isolated heart Langendorff and Neely models were established the rat hearts in Group TTX were continuously perfused with Krebs-Henseleit(K-H) buffer solution for 30 minutes,arrested by TTX cardioplegia(4℃) for 60 minutes,underwent reperfusion with K-H buffer solution for 60 minutes,and then the left ventricular samples were collected for detections.The rat hearts in Group TTX+AG490 were perfused and reperfused with JAK2 inhibitor AG490(5μmol/L) and K-H buffer solution under the same procedure as Group TTX.The protein expression indexes(PEI) of phosphorylated-STAT3(p-STAT3) and heat shock protein 70(HSP 70) in myocardium were detected by immunohistochemical assay(IHC).The apoptosis index(AI) of cardiomyocyte was detected by terminal deoxynucleotidyl transferase-mediated dUTP nick-end labeling(TUNEL).The changes of these indexes in three groups were used for comparison.Results Compared with Group Control,the PEI of p-STAT3 and HSP 70 in Group TTX and Group TTX+AG490 increased significantly(P0.05);Treated with AG490,the PEI of p-STAT3 and HSP 70 in Group TTX+AG490 was lower than that in Group TTX(P0.05).The PEI of HSP 70 had a positive correlation with the PEI of p-STAT3(r=0.826,P0.05).After ischemia/reperfusion,AI in Group TTX and Group TTX+AG490 was significantly higher than that in Group Control(P0.05);compared with Group TTX,AI in Group TTX+AG490 increased significantly(P0.05).Conclution JAK2/STAT3 pathway could mediate myocardial protection of TTX cardioplegia in rat hearts via upregulating the protein expression of HSP 70 and mobilizing of endogenous cardiac protection mechanisms.
出处
《西部医学》
2011年第3期415-418,共4页
Medical Journal of West China
