摘要
目的建立SD大鼠星形胶质细胞缺氧复氧损伤模型,探讨p38MAPK活性变化与星形胶质细胞损伤的关系。方法体外培养新生SD大鼠星形胶质细胞,实验设正常对照组(N)、SB203580组(SB组,10μmol/L)、缺氧/复氧组(H/R组)和缺氧/复氧组+SB203580阻断p38MAPK组(H/R+SB组)。应用MTT法、WB法、ELISA法检测缺氧4h、8h、复氧6h、12h、24h、48h时细胞存活率,p38MAPK、p-p38(磷酸化p38MAPK)及TNF-α的变化。结果培养星形胶质细胞GFAP阳性表达率大于97%。缺氧/复氧使星形胶质细胞活力降低,SB203580阻断p38MAPK细胞活力高于H/R组,各组星形胶质细胞总p38MAPK水平无显著变化,缺氧复氧干预后p-p38表达上调,TNF-α水平显著增高。用SB203580阻断p38MAPK通路后,SB+H/R组较H/R组p-p38、TNF-α水平降低。SB组总p38MAPK、p-p38、TNF-α水平与N组比较无显著变化。结论 p38MAPK信号通路参与了星形胶质细胞缺氧复氧损伤过程。
Objective To establish astrocytes hypoxia-reoxygenation induced injury model,observe the astrocytes impairment under hypoxic/reoxygenation and investigate the relationship between p38MAPK signaling and astrocytes induced by hypoxic/reoxygenation in vitro.Methods Reference to the methods of McCarthy,the primary cells from the cortex of SD fetal rat,the cultured astrocytes were divided into four groups: normal contrast group(N),hypoxia/reoxygenation group(H/R),SB203580 group(SB),and hypoxia/reoxygenation+the SB203580 interrupt p38MAPK group(H/R+SB).SB203580 with a final concentration of 10 μmol/L,to add in 1 hour before hypoxia.After 4,8 hours of hypoxia,it began to reoxygenation.Each group reoxygenation 6 hours,12 hours,24 hours,48 hours.MTT was used to detect the cell activity.Western-blot analysis of semi-quantitative detected the p38 and p-p38 expression.TNF-α secretion of astrocytes was measured by TNF-α ELISA.Results Homogeneity of the cell populations was evaluated by immunofluorescence examinations with ant-glia fibrillary acid protein(GFAP),the number of GFAP positive cells exceeded 97%.Hypoxia/reoxygenation reduced the astrocyte activity,cell viability was higher than the H/R group with SB203580 block p38MAPK,no significant changes in total p38MAPK level among the four groups.p-p38 expression increased after the intervention of hypoxia and reoxygenation and TNF-α level was increased.When p38MAPK pathway was inhibited by SB203580 in the H/R+SB group,the levels of p-p38 and TNF-α were reduced compared with H/R group.The levels of p38MAPK,p-p38 and TNF-α in the SB group had no changes compared with the normal group.Conclusion p38MAPK signaling pathway is involved in the process of astrocytes in hypoxia-reoxygenation injury
出处
《中国实用神经疾病杂志》
2012年第9期1-4,共4页
Chinese Journal of Practical Nervous Diseases
