大鼠视神经损伤后Bad蛋白表达与视网膜神经细胞观察

法医学杂志 ›› 2006, Vol. 0 ›› Issue (4): 258-260+.

大鼠视神经损伤后Bad蛋白表达与视网膜神经细胞观察

吴红色;柯技;陈晓瑞;

华中科技大学同济医学院法医学系,华中科技大学同济医学院法医学系,华中科技大学同济医学院法医学系湖北武汉430030,湖北武汉430030,湖北武汉430030

发布日期:2006-08-25 出版日期:2006-08-28

Changes of Retinal ganglion cells and Expression of Bad after Optic Nerve Crush in Rats

WU HONG-SE, KE JI, CHEN XIAO-RUI (DEPARTMENT OF FORENSIC MEDICINE, TONGJI MEDICAL COLLEGE OF HUAZHONG UNIVERSITY OF SCIENCE AND TECHNOLOGY, WUHAN 430030,CHINA)

Online:2006-08-25 Published:2006-08-28

摘要/Abstract

摘要： 目的观察大鼠视神经钳夹伤后视网膜神经节细胞(RGCs)和Bad蛋白表达变化。方法建立大鼠视神经钳夹伤动物模型,伤后1,3,5,7,9,14,28d处死,HE染色观察RGCs的改变,免疫组化方法检测Bad蛋白的表达水平。结果视神经损伤后1d节细胞开始减少,7d内呈快速减少,14d后呈慢速减少期,28d后趋于稳定;伤后3dBad蛋白表达明显增加,5d时达到高峰,7d后开始下降,14d后变化不明显。结论视神经损伤Bad蛋白的表达诱发RGCs丧失,是伤后视功能下降的重要原因,视功能评价应在损伤28d以后进行。

关键词: 视神经损伤, 视网膜神经节细胞, Bad, 视功能

Abstract: Objective To observe the change of retinal ganglion cells(RGCs)and the expression of Bad after optic nerve injury, so as to study the changes of optic function level on morphology and molecular. Methods The experimental models of optic nerve crush were established in fifty Wistar rats. At the different time after injuries (from one to twenty-eight day), the changes of RGCs were observed under microscope. Immunohistochemiscal technique and computer image analysis methods were performed to observe the changes of Bad in RGCs in rats. Results The number of RGCs was reduced significantly according to partial lesion of optic nerve crush. An initial loss of RGCs densities was accelerated in one week after nerve crush, two weeks later the trend mitigated. After four weeks, no obvious change were observed. The expression of Bad increased in 3 days, reached peak in 5 days, and declined one week later. No obvious changes were observed after two weeks. Conclusion The expression of Bad lead to the loss of RGCs following optic nerve crush. This is the important reason of loss optic function. The identification on optic nerve injuries should be done at least four weeks later.

Key words: optic nerve crush, retinal ganglion cells(RGCs), Bad, visual function

吴红色;柯技;陈晓瑞;. 大鼠视神经损伤后Bad蛋白表达与视网膜神经细胞观察[J]. 法医学杂志, 2006, 0(4): 258-260+.

WU HONG-SE;KE JI;CHEN XIAO-RUI (DEPARTMENT OF FORENSIC MEDICINE;TONGJI MEDICAL COLLEGE OF HUAZHONG UNIVERSITY OF SCIENCE AND TECHNOLOGY;WUHAN 000;CHINA). Changes of Retinal ganglion cells and Expression of Bad after Optic Nerve Crush in Rats[J]. , 2006, 0(4): 258-260+.

[1]	项剑, 王旭, 于丽丽, 靳康佳, 杨英恺. 视交叉及其后部视路损伤所致视野缺损的客观评定[J]. 法医学杂志, 2023, 39(4): 350-359.
[2]	戴定坤, 杨丽, 孟欢欢, 陈溪萍, 陶陆阳. 不同部位损伤致视力障碍的视觉诱发电位特征[J]. 法医学杂志, 2021, 37(5): 632-638.
[3]	项剑, 王旭, 于丽丽, 等. 应用传统VEP、多焦VEP进行视觉功能客观评定1例[J]. 法医学杂志, 2020, 36(6): 884-887.
[4]	曾铭伟，王涛，费成平,等. 大鼠视神经挫伤致视网膜硫化氢合成酶表达变化[J]. 法医学杂志, 2018, 34(6): 635-639.
[5]	刘会, 王旭. 微视野仪在视功能评估中的应用[J]. 法医学杂志, 2014, 30(3): 194-196.
[6]	彭书雅，陈捷敏，刘瑞珏，等. 多焦视觉电生理技术在视功能评估中的应用[J]. 法医学杂志, 2013, 29(4): 286-289,294.
[7]	徐传宝;胡乃平;. 高坠致视神经损伤伤残鉴定1例[J]. 法医学杂志, 2007, 0(1): 74-75.
[8]	张经伟. 视神经损伤的模式翻转视觉诱发电位24例分析[J]. 法医学杂志, 1996, 0(1): 0-0.