脑室内注射脂多糖大鼠海马部位星形胶质细胞的变化

Changes of astrocytes in the hippocampus of a model of intra-ventricular injection of lipopolysaccharide in the rat

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摘要目的研究侧脑室注射脂多糖(lipopolysaccharide,LPS)引发大鼠脑内炎性反应时,海马部位星形胶质细胞的变化。方法健康雄性SD大鼠64只,采用数字表法随机分为0.9%氯化钠注射液(normal saline,NS)对照组和LPS实验组。LPS实验组大鼠右侧脑室一次性注射LPS 20μL(1.25 g/L),NS对照组大鼠脑室内注射同等体积的NS。于注射后2、4、12及24周应用免疫组织化学染色方法观察大鼠海马部位星形胶质细胞特异性标志物-胶质原纤维酸性蛋白(glial fibrillary acidic protein,GFAP)阳性细胞的变化,并应用Western blotting方法检测大鼠海马部位GFAP蛋白表达的变化。结果 GFAP免疫组织化学染色结果显示,NS对照组大鼠不同时间点海马部位星形胶质细胞均未见明显激活。LPS实验组大鼠海马部位星形胶质细胞在LPS注射后2周明显激活,而LPS注射后4周和12周时海马部位星形胶质细胞激活不明显。LPS注射后24周时,LPS实验组大鼠海马部位星形胶质细胞又出现轻度激活。Western blotting结果显示,NS对照组大鼠不同时间点海马部位GFAP蛋白表达量无明显变化。LPS实验组大鼠海马部位GFAP蛋白表达量在LPS注射后2周时明显高于相应NS对照组,为相应NS对照组的2.39倍,差异有统计学意义(P<0.01)。而注射后4周及12周时,LPS实验组大鼠海马部位GFAP蛋白表达量与相应NS对照组相比变化不明显。到注射后24周时,LPS实验组大鼠海马部位GFAP蛋白表达量为相应NS对照组的1.19倍,差异无统计学意义(P>0.05)。结论侧脑室注射LPS可在早期(注射后2周)显著引起大鼠海马部位星形胶质细胞的急性激活。 Objective To investigate the change of astrocytes in the hippocampus in intracephalic inflammation rat model induced by intra-ventricular injection of lipopolysaccharide（LPS）. Methods Altogether 64 heahhy male SD rats were assigned into normal saline （NS）-injected group or LPS-injected group randomly. All injections were made intra-ventricularly on right side of the rats with NS 20 μL or LPS 20μL（ 1.25 g/L）. The changes of the the astrocytes in rat hippocampus were observed by immunohistochemical staining using astrocyte-specific marker-glial fibrillary acidic protein（GFAP） at 2 weeks, 4 weeks, 12 weeks and 24 weeks after NS or LPS injection. Western blot was performed to detect GFAP expression in the hippocampus of the rats. Results Immunohistochemical staining with GFAP antibody showed that the astrocytes in the hippocampus of rats were not activated at any time point after NS injection in NS-injected group. The astrocytes were activated obviously in the hippocampus of rats in LPS-injected group at 2 weeks after LPS injection. The activation of astrocytes was not found in the hippocampus in LPS-injected group at 4 and 12 weeks while the astrocytes were re-activated slightly in the hippocampus of LPS-injected group rats at 24 weeks after LPS injection. The result of Western blotting showed that the expression of GFAP in the hippocampus of NS-injected group rats did not change significantly at any time point after NS injection. The GFAP protein level in the hippocampus of LPS-injected group rats was 239% of that of NS-injected group rats at 2 weeks after injection （P〈0.01）. At 4 and 12 weeks after injection, the GFAP protein level in LPS-injected group was similar to that of NS-injected group. Theexpression of GFAP protein in the hippocampus of LPS-injected group was 119% of that of NS-injected group at 24 weeks post injection with no significant difference（P〉0.05）. Conclusion Intra-ventricular injection of LPS may result in acute and significant activation of astrocytes in the hippocampus of rats at early time（2 weeks post injection）.

作者赵咏梅吕风月徐群渊

机构地区首都医科大学宣武医院神经变性病教育部重点实验室北京市老年病医疗研究中心首都医科大学北京神经科学研究所

出处《首都医科大学学报》 CAS 2012年第6期771-775,共5页 Journal of Capital Medical University

基金国家重点基础研究发展计划(973计划)(2007CB947700) 北京市自然科学基金(7122036)~~

关键词炎性反应多巴胺能神经元海马星形胶质细胞 inflammation dopaminergic neurons hippocampus astrocyte

分类号 R592 [医药卫生—老年医学]

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参考文献13

1McGeer P L, Yasojima K, McGeer E G. Inflammation in Parkinson' s disease [ J ]. Adv Neurol, 2001,86 : 83-89.
2Hemandez-Romero M C, Delgado-Cortes M J, Sarmiento M, et al. Peripheral inflammation increases the deleterious effect of CNS inflammation on the nigrostfiatal dopaminergic system[ J ]. Neurotoxicology, 2012,33 (3) :347-360.
3Hunter R L, Dragicevic N, Seifert K, et al. Inflammation induces mitochondrial dysfunction and dopaminergic neuro- degeneration in the nigrostriatal system [ J ]. J Neurochem, 2007,100 (5) : 1375- 1386.
4赵咏梅,吕风月,许秋岩,闫颖,徐群渊.大鼠脑内炎症对黑质多巴胺能神经元的长时程毒性作用及星形胶质细胞变化[J].中华老年医学杂志,2010,29(5):416-419. 被引量：4
5赵咏梅,吕风月,徐群渊.脑源性神经营养因子在脑室注射脂多糖大鼠黑质多巴胺能神经元变性中的作用[J].首都医科大学学报,2009,30(5):648-652. 被引量：3
6Rappold P M, Tieu K. Astrocytes and therapeutics for Par- kinson' s disease [ J ]. Neurotherapeutics, 2010,7 ( 4 ) : 413-423.
7Halliday G M, Stevens C H. Glia: initiators and progres- sors of pathology in Parkinson' s disease [ J ]. Mov Disord, 2011,26( 1 ) :6 -17.
8Sidoryk-Wegrzynowicz M, Wegrzynowiez M, Lee E, et al. Role of astroeytes in brain function and disease [ J ]. Toxieol Pathol, 2011,39 ( 1 ) : 115-123.
9Braak H, Sastre M, Del Tredici K. Development of alpha- synuclein immunoreactive astrocytes in the forebrain paral- lels stages of intraneuronal pathology in sporadic Parkinson' s disease[J]. Acta Neuropathol, 2007,114(3):231-241.
10Rathinam M L, Watts L T, Narasimhan M, et al. Astrocyte mediated protection of fetal cerebral cortical neurons from rotenone and paraquat [ J ]. Environ Toxicol Pharmacol, 2012,33(2) :353-360.

二级参考文献26

1周春来,张进禄,李继梅,霍洁,薛启蓂,徐群渊.一氧化碳对脂多糖诱导大鼠纹状体炎性反应后的多巴胺能神经元的影响[J].中华老年医学杂志,2007,26(6):463-467. 被引量：1
2McGeer P L,Yasojima K,McGeer E G.Inflammation in Parkinson's disease[J].Adv Neurol,2001,86:83-89.
3Herrera A J,Castano A,Venero J L,et al.The single intranigral injection of LPS as a new model for studying the selective effects of inflammatory reactions on dopaminergic system[J].Neurobiol Dis,2000,7:429-447.
4Mocchetti I,Bachis A,Nosheny R L,et al.Brain-derived neurotrophic factor expression in the substantia nigra does not change after lesions of dopaminergic neurons[J].Neurotox Res,2007,12:135-143.
5Porritt M J,Batehelor P E,Howells D W.Inhibiting BDNF expression by antisense oligonucleotide infusion causes loss of nigral dopaminergic neurons[J].Exp Neurol,2005,192:226-234.
6Gao H M,Jiang J,Wilson B,et al.Micraglial activationmediated delayed and progressive degeneration of rat nigral dopaminergic neurons:relevance to Parkinson's disease[J].J Neurochem,2002,81:1285-1297.
7Sohrabji F,Lewis D K.Estrogen-BDNF interactions:implications for neurodegenerative diseases[J].Front Neuroendocrinol,2006,27:404-414.
8Fumagalli F,Racagni G,Riva M A.Shedding light into the role of BDNF in the pharmacotherapy of Parkinson's disease[J].Pharmacogenomics J,2006,6:95-104.
9Howells D W,Porritt M J,Wong J Y F,et al.Reduced BDNF mRNA expression in the Parkinson's disease substantia nigra[J].Exp Neurol,2000,166:127-135.
10Siegel G J,Chauhan N B.Neurotrophic factors in Alzheimer's and Parkinson's disease brain[J].Brain Res Rev,2000,33:199-227.

共引文献5

1赵咏梅,吕风月,许秋岩,闫颖,徐群渊.大鼠脑内炎症对黑质多巴胺能神经元的长时程毒性作用及星形胶质细胞变化[J].中华老年医学杂志,2010,29(5):416-419. 被引量：4
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3何怡瀚,于涛.针刺治疗帕金森病对脑内神经元再生影响的研究进展[J].新中医,2012,44(1):106-108.
4刘扬,史明,杜可军,张鹏,赵钢.HLRP蛋白在大鼠脑中的定位及LPS对其表达的影响[J].现代生物医学进展,2012,12(10):1801-1804.
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2高健,刘振.多巴胺能神经元替代治疗帕金森病的研究进展[J].中华神经医学杂志,2005,4(6):642-645. 被引量：2
3罗超,程德森,彭吉霞,何华琼.侧脑室内注射葛根素对大鼠血压和心率的影响[J].大同医学专科学校学报,2004,24(2):18-19. 被引量：2
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7李大伟,赵晓民,张玲,蔡洪信,夏青,杨明峰,夏作理.糖尿病对大鼠脑内葡萄糖转运蛋白表达的影响[J].中国糖尿病杂志,2008,16(12):755-756. 被引量：3
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脑室内注射脂多糖大鼠海马部位星形胶质细胞的变化

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