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大鼠脊髓全横断后TrkA和NGF在运动皮质的免疫组化研究 被引量:5

The Immunohistochemical Study of TrkA and NGF in Adult Rat Motor Cortex Following Spinal Cord Complete Transection
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摘要 目的 探讨脊髓全横断后神经营养因子及相应受体在运动皮质内的分布规律 ,为临床应用神经生长因子治疗脊髓损伤提供实验依据。方法 用免疫组化方法和图像分析技术检测脊髓全横断后不同时相运动皮质内 ,神经生长因子 (NGF)及其高亲和性受体TrkA的表达和分布。结果 各组运动皮质中TrkA和NGF阳性神经元主要分布在第 5层 ;脊髓全横断 3d后 ,运动皮质内TrkA表达上调 ,损伤后 7d到达高峰 ,2 1d回到正常水平 ;NGF表达在损伤后 7d上调 ,峰值出现在损伤后 7d ,2 1d回到正常水平。结论 NGF表达增高迟于TrkA 。 Objective To study the pattern of the distribution of neurotrophin receptors tyrosine kinase A(TrkA) and nerve growth factor (NGF) in adult rat motor cortex following complete spinal cord transection (SCT). Methods With immunohistochemistry and quantitative analysis, the expression and distribution of neurotrophin receptors TrkA and NGF were detected in motor cortex following complete SCT. Results TrkA and NGF immunoreactive positive cells are mainly localized in motor cortex layer V in both control and experimental groups. The expression of TrkA in adult rat motor cortex was up-regulated after transection in day 3 and reached the peak in day 7; While the expression of NGF in motor cortex was up-regulated and reached the peak in day 7 after transection. Conclusion The up-regulation of NGF occurred earlier than that of NGF, the results suggest that administration of exogenous NGF may be beneficial for the survival and regeneration of the injured corticospinal neurons in the early period after injury.
作者 万炜 何洁 陈熙 李学军 邓盘月 罗学港
机构地区 南华大学解剖学教研室 南华大学病理学教研室 中南大学湘雅医院 中南大学神经生物学研究室
出处 《南华大学学报(医学版)》 2003年第3期257-259,274,共4页 Journal of Nanhua University(Medical Edition)
基金 国家重点基础研究规划"脑功能和脑重大疾病的基础研究"(G19990 5 40 0 9)项目资助
关键词 大鼠 脊髓全横断 TRKA NGF 运动皮质 免疫组化 神经营养因子 脊髓损伤 spinal cord complete transection TrkA NGF motor cortex
分类号 R651.2 [医药卫生—外科学]
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参考文献12

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  • 2万祎,陈熙,何洁,邓盘月,罗学港.NGF和BDNF在脊髓全横断后大鼠运动皮质的表达和分布[J].南华大学学报(医学版),2003,31(1):1-4. 被引量:3
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二级参考文献12

  • 1Yan Q, Radeke MJ, Metheson CR, et al. Immunocytochemical localization of TrkB in the certral nervons system the adult rat [ J]. J Comp Neurol , 1997,378 : 135 - 137.
  • 2Ye JH, Houle JD. Treatment of athe chronically injured spinal cord with neurotrophic factors can promote axonal regeneration from supraspinal neurons [ J ]. Exp Neurol,1997,143:70 - 81.
  • 3Te Talaff, Kobayashi WNR, Giehl KMG, et al. Response of rubraspinal and corticospinal neurons to injury and neurotrophim prog[ J]. Brain Res, 1994,103:271 - 286.
  • 4Michael GJ, Averill S, Nitkunan A, et al. Nerve growth factor treatment increase brain- derived neurotrophic factor selectively in trkA- expressing dorsal root ganglion cells and in their central terminations with in the spinal cord[ J]. J Neurosci, 1997,17 : 8476 - 8490.
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  • 6Li LR,Dppenheim RW,Lei M, et al. Neurotrophic factors rescue mouse motoneurons from naturally occuring and axotomy - induced cell death[ J]. Soc Neurosci, 1993, 19:1099.
  • 7Kobayashi NR, Fan DP, Giehl KM, et al. BDNF and NT-4/5 prevent atrophy of rat rubraspinal neurons after cervical axotomy, stimulate GAP - 43 and Talphal - tubulin mRNA expression, and promote axonal regeneration[ J ]. J Neurosci, 1997,17(24) :9583 - 9595.
  • 8Kramer LF. Nerve growth factors treatment after brain injury prevert neuronal death[J]. Science, 1996,235:214.
  • 9Blochl A , Thoenen H. Characterization of nerve growth factor release from laippocompal neuron: evidence for a constitutive and an tmconvertiona], sodium- dependent regulater pathway[J]. Eur J Neuroses, 1995,7:1220 -1228.
  • 10Altar CA, Siuciak JA, Wright P, et al. Insitu hybridization of TrkB and Trkc receptor mRNA in rat forebrain and association with high affinity binding of 125 IBDNF, 125INT-4/5, and 125 INT- 3 [ J]. Ettr J Neurosci, 1994,6:1389 -1405.

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二级引证文献13

南华大学学报(医学版)
2003年 第3期

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