摘要
目的:探讨地塞米松对海人酸致痫大鼠脑P-糖蛋白(P-gp)表达的影响.方法:将SD大鼠随机分为假手术组(Sham组,n=8)、癫痫组(EP组,n=12)、地塞米松干预癫痫组(DEX组,n=12).后两组采用海马注射海人酸方法制作癫痫模型,DEX组癫痫造模前30 min给予腹腔注射地塞米松0.4 mg/kg.分别记录各组大鼠达到Ⅲ级和Ⅴ级发作时所需的时间(潜伏期),初次至第6次≥Ⅳ级发作的间隔时间作为评价癫痫发作严重程度的指标;大鼠术后24 h处死,使用HE染色和免疫组织化学方法,比较各组海马CA3区、齿状回、杏仁核复合体区P-gp表达及脑损伤情况.结果:①Sham 组未见癫痫发作;DEX组与EP组达到Ⅲ级发作的潜伏期分别为(87.92±45.80)min和(67.50±22.91)min,达到Ⅴ级发作的潜伏期分别为(103.33±51.27 )min和(75.60±22.10)min,差异均无统计学意义(P〉0.05);与EP组相比,DEX组样发作严重程度降低(P=0.004);②与EP组相比,DEX组于所观察的脑区损伤均减轻,以海马CA3区和杏仁核复合体区较为显著;③与Sham组比较,EP组各观察脑区P-gp表达均明显升高(P〈0.01);与EP组相比,DEX组海马CA3区和杏仁核复合体区P-gp表达显著减少(P〈0.05),而在齿状回表达量差异无统计学意义(P=0.078).结论:地塞米松可降低海人酸致痫大鼠发作严重程度和脑损伤,抑制P-gp表达上调,其中以海马CA3区和杏仁核区较为显著.
Objective:To investigate the effect of dexamethasone on P-glycoprotein (P-gp) expres sion in rats with brain kainic acid(KA) epilepsy. Methods.. SD rats were randomly divided into the shamoperated group (Sham group,n 8),the epilepsy group (EP group,n=12),and the epilepsy rats intervened with dexamethasone (DEX group,n=12). The epilepsy rats veceived KA injection and the rats of DEX group received intraperitoneal injection of dexamethasone(0.4 mg/kg)30 min prior to KA. The latency to Grade Ⅲ and Ⅴ onset of each group were recorded as well as the frequency of severe seizures. All rats were killed 24 h after KA treatment. HE staining and immunohistochemical methods were used to compare the differences of P-gp expression in the hippoeampal CA3 area, dentate gyrus,and amygdala complex area and brain damage. Results: (1)No seizures were observed in Sham group. The latency to Grade Ⅲ onset in DEX and EP groups were (87.92 ± 45.80)min and (67. 50 ± 22. 91)min, and to Grade V onset were (103.33 ± 51. 27)min and (75.60± 22.10)minrespectively. There was no statistical difference (P〉0.05). Compared with EP group, the severity of epileptic seizures of DEX group decreased (P=0. 004). (2)Compared with EP group, the damage of epileptic related brain areas in DEX group was reduced. (3)A small amount of P-gp was expressed in the brains of Sham group. The P-gp expression of EP group was significantly enhanced (P〈0.01). Compared with the EP group, P-gp expression in hippocampus CA3 area and the arnygdala complex of DEX group was significantly reduced (P〈0.05), but there was not significant difference in dentate gyrus (P〈0. 078). Conclusion: Dexamethason ecan reduce seizure severity and brain damage of epileptic rats and block up regulation of P-gp in the rat brain.
出处
《癫痫与神经电生理学杂志》
2010年第5期262-266,共5页
Journal of Epileptology and Electroneurophysiology(China)
基金
南京市医学科技发展重大项目(2007-0211)
