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托吡酯治疗兔的视网膜功能和组织病理学

Retinal function and histopathology in rabbits treated with Topiramate.

作者信息

Kjellström S, Bruun A, Isaksson B, Eriksson T, Andréasson S, Ponjavic V

机构信息

Department of Ophthalmology, University of Lund, S 221 85, Lund, Sweden.

出版信息

Doc Ophthalmol. 2006 Nov;113(3):179-86. doi: 10.1007/s10633-006-9027-8. Epub 2006 Nov 18.

Abstract

PURPOSE

To evaluate retinal function and histopathology in rabbits treated orally with the anti-epileptic drug topiramate.

METHODS

Six rabbits were treated with a daily oral dose of topiramate during a period of eight months. Six rabbits receiving water served as controls. Blood samples were analyzed for determination of topiramate serum levels in order to ensure successful drug exposition. Standardized full-field electroretinograms (ERGs) were performed before treatment and then at 2, 3 and 8 months during the treatment period. After terminating treatment the rabbits were sacrificed and the morphology of the sectioned retina was studied.

RESULTS

After eight months of treatment the full-field ERG demonstrated normal rod function in treated and control rabbits, but the light adapted 30 Hz flicker b-wave amplitude was significantly reduced in the treated rabbits. This was the case for both the light adapted (Wilcoxon signed ranks test, P = 0.046) and the dark adapted (Wilcoxon signed ranks test, P = 0.028) 30 Hz flicker response from the treated rabbits. Retinal immunohistology revealed a severe accumulation of GABA in amacrine cells and in the inner plexiform layer in 4 of 6 treated rabbits compared to the controls.

CONCLUSIONS

Topiramate, orally administrated to rabbits, may cause a significant reduction of the retinal function demonstrated by the reduced b-wave amplitude in the full-field ERG, as well as changes in immunohistology characterized by a severe accumulation of GABA in the inner retina. The retinal dysfunction and the morphological changes indicate that topiramat may damage the retina, similarly to vigabatrin (another anti-epileptic drug).

摘要

目的

评估口服抗癫痫药物托吡酯治疗的家兔的视网膜功能和组织病理学变化。

方法

6只家兔在8个月期间每日口服托吡酯。6只饮用纯水的家兔作为对照。分析血样以测定托吡酯血清水平,以确保药物暴露成功。在治疗前以及治疗期间的第2、3和8个月进行标准化的全视野视网膜电图(ERG)检查。治疗结束后处死家兔,研究视网膜切片的形态。

结果

治疗8个月后,全视野ERG显示治疗组和对照组家兔的视杆功能正常,但治疗组家兔的明适应30Hz闪烁b波振幅显著降低。治疗组家兔的明适应(Wilcoxon符号秩检验,P = 0.046)和暗适应(Wilcoxon符号秩检验,P = 0.028)30Hz闪烁反应均出现这种情况。视网膜免疫组织学显示,与对照组相比,6只治疗组家兔中有4只的无长突细胞和内网状层中GABA严重积聚。

结论

给家兔口服托吡酯可能会导致全视野ERG中b波振幅降低所显示的视网膜功能显著下降,以及免疫组织学变化,其特征为视网膜内层GABA严重积聚。视网膜功能障碍和形态学变化表明,托吡酯可能会像另一种抗癫痫药物氨己烯酸一样损害视网膜。

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