期刊文献+
任意字段
题名或关键词
题名
关键词
文摘
作者
第一作者
机构
刊名
分类号
参考文献
作者简介
基金资助
栏目信息

不同浓度瑞芬太尼对乳鼠离体脑海马神经细胞存活和凋亡的影响 被引量:2

Effect of different concentrations of remifentanil on hippocampal neuron apoptosis in vitro
在线阅读 下载PDF
导出
摘要 目的探讨不同浓度瑞芬太尼对乳鼠离体脑海马神经细胞存活及凋亡的影响。方法原代培养乳鼠脑海马神经细胞:取出生7d的新生乳鼠海马神经细胞,原代培养7d,随机分为正常对照组(G组);瑞芬太尼72ng/ml处理组(R1组);瑞芬太尼126ng/ml处理组(R2组);瑞芬太尼180ng/ml处理组(R3组)。采用MTT检测脑海马神经细胞存活率、凋亡率,在电镜下观察海马神经细胞超微结构的变化。结果与G组相比较,R1、R2、R3组神经细胞存活率均降低(P<0.05),其中R2、R3组神经细胞存活率显著降低(P<0.01);R1、R2、R3组内比较海马神经细胞存活率随瑞芬太尼浓度的升高而降低(P<0.05或P<0.01)。与G组比较,R1、R2、R3组海马神经细胞凋亡率明显增加(P<0.05),其中R2、R3组神经细胞凋亡率显著增加(P<0.01);R1、R2、R3组内比较海马神经细胞凋亡率随瑞芬太尼浓度的升高而增加(P<0.05或P<0.01)。G组胞浆内细胞器结构正常。R1、R2、R3组可见不同程度的神经细胞损伤,细胞器相互靠近,其中R2、R3组神经细胞损伤程度更重,出现空泡样变性(空穴现象)。结论在本研究的浓度范围内,瑞芬太尼可抑制新生乳鼠海马神经细胞的存活并促进其凋亡,并且浓度越高,抑制其存活及促进其凋亡的作用越明显。 Objective To investigate the effect of remifentanil with different concentrations on the cell viability and apoptosis in primary cultured hippocampal neurons of neonatal rat. Methods For the primary culture hippocampal neurons in neonatal rat, primary culture hippocampal neurons isolated from newborn SD rats (7days) and cultured 7 days and then randomly divided into 4 groups: group control (group G), group remifentanil 72 ng/ml (group R1), group remifentanil 126 ng/ml (group R2), group remifentanil 180 ng/ml (group R3). The hippocampal neurons cell histopathological changes were observed with electron microscopy. The apoptosis were measured by flow cytometry and the survival of these cells were determined using MTT [3-(4, 5-two methylic thiazole-2)-2, 5-two phenyltetrazole bromide salts]. Results The neuronal viability was lower(P〈 0.05) in the groups R1, R2, and R3 when compared to the group G, and there was significantly difference in the parameter mentioned above between groups R2 and R3 (P〈0.01). The apoptosis rate of hippocampal neurons was higher (P〈0.05) in the groups R1, R2, R3 than in group G, and there was significantly difference in the parameter mentioned above between groups R2 and R3 (P〈 0.01). Regards the histopathologicaI changes of neurons ceils, the mass of organdies structure was normal in group G, however, different degrees damage of nerve cell and organdies near each other were appeared in groups R1 ,R2,R3 after drug treatment. The hippocampal neurons changes were even worse and appear empty bubble sample degeneration (cavitation) in groups R2, R3. Conclusion Remifentanil can inhibit the cell survival and promote apoptosis of neonatal rat hippocampal neurons in the study within the scope of concentratiorr It was positive related to the concentration.
作者 杨剑 商瑜 严莉 高鸿
机构地区 贵阳医学院附属医院麻醉科 山东省滨州市人民医院麻醉科 贵阳医学院附属白云医院麻醉科
出处 《临床麻醉学杂志》 CAS CSCD 北大核心 2013年第9期902-904,共3页 Journal of Clinical Anesthesiology
基金 贵州省卫生厅科学技术基金项目(gzwkj 2011-1-062)
关键词 瑞芬太尼 海马 神经细胞 细胞凋亡 Remifentanil Hippocampal Nerve ceils Ceil apoptosis
分类号 R726.1 [医药卫生—儿科]
  • 相关文献

参考文献11

二级参考文献37

  • 1俞文军.瑞芬太尼的靶控输注在自主呼吸短小手术病人中的应用[J].中国临床医学,2005,12(1):159-161. 被引量:9
  • 2黄悦,杭燕南.小儿瑞芬太尼药动学及临床研究进展[J].国外医学(麻醉学与复苏分册),2005,26(2):114-117. 被引量:81
  • 3Andersson C, Blennow K, Almkvist O, et al. Increasing CSF phospho-tau levels during cognitive decline and progression to dementia. Neurobiol Aging, 2008, 29: 1466-1473.
  • 4Ferrer-Alco'n M, La Harpe R, Guimo'n J, et al. Downregulation of Neuronal cdkS/p35 in opioid addicts and opiate-treated rats: relation to neurofilament phosphorylation. Neuro psychopharmacology, 2003, 28:947-955.
  • 5Liu M, Choi S, Cuny GD, et al. Kinetic studies of Cdk5/p25 kinase: phosphorylation of tau and complex inhibition by two prototype inhibitors. Biochemistry, 2008, 47 : 8367-8377.
  • 6Shahani N, Brandt R. Functions and malfunctions of the tau proteins. Cell Mol Life Sci, 2002, 59: 1668-1680.
  • 7Zhou XW, Li X, BjorkdahlC, et al. Assessments of the aecu mulation severities of amyloid beta protein and hyperphosphorylated tau in the medial temporal cortex of control and Alzheimer's brains. Neurobiol Dis, 2006, 22: 657-668.
  • 8Gong CX, I.iu F, Grundke Iqbal I, et al. Post translational modifications of tau protein in Alzheimer's disease. J Neural Transm, 2005, 112:813-838.
  • 9Tsai I.H, Lee MS, Cruz J. Cdk5, a therapemic target for Alzheimer's disease? Biochim Biophys Acta,2004, 1697: 137- 142.
  • 10Paus T. Functional anatomy of arousal and attention systems in the human brain. Prog Brain Res, 2000, 126:65 77.

共引文献36

同被引文献19

  • 1黄继汉,黄晓晖,陈志扬,郑青山,孙瑞元.药理试验中动物间和动物与人体间的等效剂量换算[J].中国临床药理学与治疗学,2004,9(9):1069-1072. 被引量:1423
  • 2丁汉琳,张咸伟,张传汉.芬太尼影响MCF7细胞凋亡的实验研究[J].实用医学杂志,2004,20(12):1351-1353. 被引量:16
  • 3刘志恒,高峰,田玉科.吗啡、芬太尼、曲马多对Jurkat细胞核因子κB和IL-2合成的影响[J].中国医院药学杂志,2007,27(5):579-582. 被引量:10
  • 4Vadalouca A,Moka E,Argyra E,et al.Opioid rotation in patients with cancer:a review of the current literature.J Opioid Manag,2008,4(4):213-250.
  • 5Clark MJ,Robien K,Slavin JL.Efect ofprebintics on biomarkers of colorectal cancer in humans:a systematic review.Nutr Rev,2012,70(8):436-443.
  • 6Davis PJ,Finkel JC,Orr RJ,et al.A randomized,double-blind study of remifentanil versus fentanyl for tonsillectomy and adenoidectomy surgery in padiatric ambulatory surgical patients.Anesth Analg,2000,90(4):863-871.
  • 7Nav~Mesa MO, Lamprea MR, M(mera A. Divergent short- and long-term effects of acute stress in object recognition memory are mediated by endogenous opioid system activation. Neurobiol Learn Mem, 2013, 106:185-192.
  • 8Irwin MG, Wong GT. Remifentanil and Opioid-Induced Car- dioprotection. J Cardiothoracic Vasc Anesth, 2015, 29(Suppl 1) :$23-$26.
  • 9Kida S. A functional role for CREB as a positive regulator of memo- ry formation and LTP. Exp Neurobiol, 2012,21(4):136-140.
  • 10Haghparast A, Taslimi Z, Ramin M, et al.Changes in phospho- rylation of CREB, ERK, and c-fos induction in rat ventral teg- mental area, hippocampus and prefrontal cortex after conditioned place preference induced by chemical stimulation of lateral hypo- thalamus.Behav Brain Res, 2011,220(1) .. 112 118.

引证文献2

二级引证文献15

临床麻醉学杂志
2013年 第9期

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部