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机构地区:[1]内蒙古医学院病理教研室,内蒙古呼和浩特010059
出 处:《内蒙古医学院学报》2011年第5期387-391,共5页Acta Academiae Medicinae Neimongol
基 金:内蒙古教育厅研究课题(NJZY07093)
摘 要:目的:观察外源性给予改构体酸性成纤维细胞生长因子(aFGF)后,肠缺血-再灌注损伤中转录因子AP-1(fos/jun复合物)表达规律。方法:以大鼠肠系膜上动脉(SMA)夹闭造成肠缺血-再灌注损伤模型,并将动物随机分为假手术组(C)、生理盐水对照组(R)、改构体治疗组(F)。除假手术组外,其余各组动物均于缺血45 min后2、6、12、24h活杀,取小肠组织标本,免疫组化检测原癌基因c-fos、c-jun表达规律。结果:在正常大鼠,原癌基因c-fos、c-jun分布在小肠绒毛上皮细胞的肠腔侧、侧壁和小肠隐窝朝向隐窝腔的一侧的细胞膜上。缺血和再灌注的初期,原癌基因c-fos、c-jun的表达未发生明显变化,随着再灌注时间的延长逐渐增强。改构体aFGF使原癌基因c-fos、c-jun的表达有明显的增强。缺血和再灌注使PCNA的表达增加,在再灌注后6 h达到高峰。F组PCNA的表达较R组相应时间点显著增加(P<0.05)。结论:转录因子AP-1与PCNA表达一致,在缺血-再灌注损伤的修复中起积极作用;改构体aFGF对此有促进作用。Objective:To investigate the influences of exogenous acidic fibroblast growth factor(aFGF) on the AP-1(fos/jun complex) expression in rat intestine ischemia-reperfusion injury model.Methods:Rat gut I-R injury models were established by clamping the superior mesenteric artery(SMA),and the animals were divided randomly into sham-operation group(C),saline control group(R) and aFGF treatment group(F).The expression level of c-fos、c-jun and PCNA were measured with immuno-histology and semi-quantification with MIG2000 combined graphic analytic system at 2,6,12 and 24h after clamping and reperfusion.Results: The expression of c-fos、c-jun remained unchanged at the early stages of the injury but increased gradually with the prolonging of reperfusion in the control group;while the expression level of c-fos、c-jun and PCNA was significantly increased and reached its peak at 6h in the treatment group(P〈0.05).Conclusions:The expression of AP-1 is closely related to that of PCNA and plays a positive role in the I-R injury repair process which is enhanced by aFGF.
关 键 词:改构体酸性成纤维细胞生长因子 转录因子AP-1 缺血-再灌注损伤
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