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血红素氧合酶系统对一氧化碳中毒后体外培养少突胶质细胞Nogo-A的影响
引用本文:王晓虹,王苏平,车菊华,王 虹,王 翠,汪 涛,朱艳玲. 血红素氧合酶系统对一氧化碳中毒后体外培养少突胶质细胞Nogo-A的影响[J]. 中国组织工程研究, 2016, 20(2): 230-235. DOI: 10.3969/j.issn.2095-4344.2016.02.014
作者姓名:王晓虹  王苏平  车菊华  王 虹  王 翠  汪 涛  朱艳玲
作者单位:大连市中心医院,神经内科,综合病房,康复科,辽宁省大连市 116033;大连医科大学,辽宁省大连市 116044;大连市第三人民医院神经内科,辽宁省大连市 116033
基金项目:大连市卫生局2008年度科研计划项目
摘    要:

关 键 词:组织构建  组织工程  一氧化碳中毒  少突胶质细胞  Nogo-A  血红素加氧酶1  锌原卟啉9  聚合酶链反应  免疫组织化学  气体信使  
收稿时间:2015-11-07

Effect of hemeoxygenase system on Nogo-A expression in rat oligodendrocytes in vitro after carbon monoxide poisoning
Wang Xiao-hong,Wang Su-ping,Che Ju-hua,Wang Hong,Wang Cui,Wang Tao,Zhu Yan-ling. Effect of hemeoxygenase system on Nogo-A expression in rat oligodendrocytes in vitro after carbon monoxide poisoning[J]. Chinese Journal of Tissue Engineering Research, 2016, 20(2): 230-235. DOI: 10.3969/j.issn.2095-4344.2016.02.014
Authors:Wang Xiao-hong  Wang Su-ping  Che Ju-hua  Wang Hong  Wang Cui  Wang Tao  Zhu Yan-ling
Affiliation:Department of Neurology, Comprehensive Ward, Department of Rehabilitation, Dalian Municipal Central Hospital, Dalian 116033, Liaoning Province, China;Dalian Medical University, Dalian 116044, Liaoning Province, China; Department of Neurology, the Third People’s Hospital of Dalian, Dalian 116033, Liaoning Province, China
Abstract:BACKGROUND: Cerebral white matter demyelination is outstanding in the images of delayed encephalopathy after acute carbon monoxide (CO) poisoning. Since Nogo-A and Nogo-receptor are expressed in onoligodendrocytes and neurons respectively, we infer that Nogo-A system is involved in brain injury after acute CO poisoning and related to delayed encephalopathy after acute CO poisoning. Endogenous CO is a gaseous messenger, which is the metabolic product of hemeoxygenase. There is no report about the CO effect on Nogo-A system till now.OBIECTIVE:To in vitro culture oligodendrocytes using endogenous CO, inhibit the activity of hemeoxygenase system using zinc protoporphyrin-IX (ZnPPIX) and observe the variation of Nogo-A in oligodendrocytes at mRNA and protein levels.METHODS:Rat oligodendrocytes cultured in vitro were divided into control, CO, ZnPPIX groups. Cells in the CO and ZnPPIX groups were treated with 1% CO directly, In the ZnPPIX group, 10 μmol/L ZnPPIX was added into the culture medium before CO treatment. The expressions of Nogo-A mRNA and protein at 6, 24, 48 hours after culture were compared. Differences in the peak levels of Nogo-A mRNA and protein between CO and ZnPPIX groups were detected using RT-PCR and immunohistochemistry respectively.RESULTS:The expression levels of Nogo-A mRNA and protein were significantly higher in the CO group than the control group and reached the peak at 24 hours of culture. Compared with the CO group, oligodendrocytes cultured with ZnPPIX showed higher expressions of Nogo-A mRNA and protein at 24 hours of culture. These findings suggest that except the influence of hypoxia occurring in CO poisoning, exogenous CO increases the expression of Nogo-A in cultured oligodendrocytes in vitro, and the heme oxygenase system can inhibit the expression of Nogo-A mRNA and protein.
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