补阳还五汤对脑缺血再灌注大鼠皮质神经细胞凋亡的影响被引量：29

Influence of Buyang Huanwu decoction on brain cortex apoptosis of cerebral ischemia and reperfusion rats

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摘要目的　研究补阳还五汤对脑缺血再灌注大鼠皮质神经细胞凋亡的影响。方法　将 36只SD大鼠随机分为 3组 :假手术组 (P ,n =12 )、模型对照组 (C ,n =12 )、补阳还五汤组 (B ,n =12 )。线栓法制作大鼠脑缺血再灌注模型 ,脑缺血再灌注 4 8h后TTC染色计算脑梗死体积 ,TUNEL染色检测神经细胞凋亡 ,免疫组化方法检测缺血侧皮质Bcl- 2 /Bax的表达 ,电镜观察线粒体的变化。结果　脑缺血再灌注后缺血侧皮质神经细胞凋亡增多 ,同时Bcl- 2表达减少 ,Bax表达增多 ,Bcl- 2 /Bax比值下降 ,线粒体肿胀且大多破裂。补阳还五汤干预后 ,细胞凋亡减少 ,脑梗死体积减小 ,Bcl- 2 /Bax比值上升 ,线粒体肿胀减轻。结论　补阳还五汤可能通过抑制神经细胞凋亡而减小脑梗死体积 ,其机制可能是通过上调Bcl- 2 /Bax比值 ,保护线粒体 ,防止发生线粒体通透性转变。 Objective It is to study the influence of Buyang Hua nwu decoction on b rain cortex apoptosis of cerebral ischemia and reperfusion rats. Methods 36 SD r ats were randomly divided into sham-operation group (P, n=12), control grou p (C, n=12) and Buyang Huanwu decoction group (B,n=12). Cerebral ischem ia and reperf usion rat models were made using the method of thread inserting right middle cer ebral artery occlusion. The infarct volume was measured 48 hours after reperfusi on. At the same time, the apoptosis was detected by TUNEL dyeing. The expression of Bcl-2 and Bax in different groups was detected by means of immunohistochemis try. The change of mitochondrion was observed with electriomicroscopic. Results The apoptosis in ischemic brain cortex was increased and the expre ssion of Bcl-2 was decreased and Bax was increased. The ratio of Bcl-2/Bax was decreased. The swelled mitochondria were lightened. When the model rats were interfered by Buya ng Huanwu decoction, the apoptosis decreased, the brain infarct volume di minished, the ratio of Bcl-2/bax increased, and the swelled mitochondria w as lightened. Conclusion Buyang Huanwu decoction can diminish brain infarct vol ume possibly b y inhibiting apoptosis. The mechanism may be increasing the ratio of Bcl-2/bax, protecting the mitochondrion and preventing the mitochondrion permeability trans ition.

作者王新高童萼塘孙圣刚

机构地区首都医科大学附属北京天坛医院华中科技大学同济医学院附属协和医院

出处《现代中西医结合杂志》 CAS 2005年第3期306-309,共4页 Modern Journal of Integrated Traditional Chinese and Western Medicine

关键词脑缺血再灌注损伤补阳还五汤细胞凋亡 BCL-2/BAX 线粒体通透性转变(MPT) cerebral ischemia and reperfusion Buyang Huanwu decoc tion apoptosis Bcl-2/Bax mitochondrion permeability transition

分类号 R-332 [医药卫生]

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1王新高,孙圣刚,童萼塘.线粒体通透性转变与缺血性脑损伤[J].国外医学（脑血管疾病分册）,2002,10(1):78-80. 被引量：2
2Green DR,Reed JC. Mitoclaondria and apoptosis[J]. Science, 1998,281(5381) :1309 - 1312. 被引量：1
3Cardoso CM,Almeida LM, Custodlo JB. Protection of tamoxifen against oxidation of mitochondrial thiols and NAD(P)H underlying the permeability transition induced by prooxidants[J]. Chem Biol Interact,2004,148(3) : 149 - 161. 被引量：1
4Ferrer l,Lopez E,Blanco R,et al. Bcl - 2,Bax,and Bcl- x expression in the CA1 area of the hippocampus following transient forebrain ischemia in the adult gerbil[J]. Exp Brain Res, 1998, 121(2) : 167 - 173. 被引量：1
5Lawrence MS, Mclaughlin JR, Sun GH, et al. Herpes simplex viral vectors expressing Bcl- 2 are neruoprotective when delivered after a stroke[J]. J Cereb Blood Flow Metab,1997~17(7) :740 - 744. 被引量：1
6Antonawich FJ, Federoff HJ, Davis IN. Bcl - 2 transduction, using a herpes simplex vires amplicon, protects hippocampal neurons from transient global ischemia[ J ]. Exp Neurol, 1999,156(1) : 130 - 137. 被引量：1
7Korsmeyer SJ. Bcl2 gene family and the regulation of programmed cell death[J]. Cancer Res, 1999,59(7):1693- 1700. 被引量：1
8Cao GD, Minami M, Pei W, et al. Intraeellular bax translocation after transient cerebral ischemia: implications for a role of the mitochondreal apoptotic signaling pathway in ischemic neuronal death[J]. J Cereb Blood Flow Metab,2001,21(4) :321-333. 被引量：1
9Adams JM,Cory S. The Bcl- 2 protein family:arbiters of cell survival[J]. Science, 1998,281(5381) : 1322 - 1326. 被引量：1
10Yin XM,Oltvai ZN, Korsmeyer SJ. BH1 and BH2 domains of Bcl -2 are required for inhibition of apoptosis and heterodimerization with Bax[J]. Nature, 1994,369(6478) :321 - 323. 被引量：1

二级参考文献23

1Kroemer G, Zamzami N, Susin SA. Mitochondrial control of apoptosis. lmmunol Today, 1997, 18(1 ): 44-51. 被引量：1
2Petit PX, Susin SA, Zarnzami N, et al. Mitochondria and programmed cell death: back to the future. FEBS Lett, 1996, 396(1): 7-13. 被引量：1
3Xu X, Decker W, Sampson MJ, et al. Mouse VDAC isoforms expressed in yeast: channel properties and their roles in mitochondrial outer membrane permeability. J Membr Biol,1999, 170(2): 89-102. 被引量：1
4Wu S, Sampson M J, Decker WK, et al. Each mammalian mitochondrial outer membrane porin protein is dispensable: effects on cellular respiration. Biochim Biophys Acta, 1999, 1452(1): 68-78. 被引量：1
5Neumar RW. Molecular mechanisms of ischemic neuronal injury. Ann Emerg Med, 2000, 36(5): 483-506. 被引量：1
6Green DR, Reed JC. Mitochondria and apoptosis. Science, 1998, 281(5381): 1309-1312. 被引量：1
7Piantadosi CA, Zhang J. Mitochondrial generation of reactive oxygen species after brain ischemia in the rat. Stroke, 1996, 27(2): 327-332. 被引量：1
8Kristian T, Siesjo BK. Calcium in ischemic cell death. Stroke, 1998, 29(3): 705-718. 被引量：1
9Nieminen AL, Petrie TG, Lemasters J J, et al. Cyclosporin A delays mitochondrial depolarization induced by N-methyl-D-aspartate in cortical neurons: evidence of the mitochondrial permeability transition.Neuroscience, 1996, 75(4): 993-997. 被引量：1
10Kristal BS, Dubinsky JM Mitochondrial permeability transition in the central nervous system: induction by calcium cycling-dependent and independent pathways. J Neurochem, 1997, 69(2): 524-538. 被引量：1