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成年大鼠再生视网膜神经节细胞的长期形态学稳定。

Long-term morphometric stabilization of regenerating retinal ganglion cells in the adult rat.

机构信息

Institute of Experimental Ophthalmology, University of Muenster, Germany.

出版信息

Restor Neurol Neurosci. 2011;29(2):127-39. doi: 10.3233/RNN-2011-0586.

Abstract

PURPOSE

Adult retinal ganglion cells (RGCs) can regenerate their cut axons within peripheral nerve grafts used to replace the distal optic nerve stump. We examined the long-term stabilization of RGCs by guiding their regenerating axons into different termination areas.

METHODS

The optic nerve (ON) of adult rats was completely cut intraorbitally and its ocular stump was connected with different visual target areas (cortex, midbrain) or with non-visual areas (e.g. muscle). Control groups consisted of blind ending graft and ON cut without graft. The function of the retina was regularly examined by electroretinography. At one, six and nine months postsurgery RGCs were retrogradely labelled with 4-(4-(didecylamino)styryl)-N-methylpyridinium iodide and examined morphometrically. Regenerating RGCs were categorized into three major classes representing the morphological types I, II and III.

RESULTS

Our data show that regenerating RGCs remain stable up to nine months after grafting at the ON, although the numbers of axons are low, that is less than 1%, and this number is not significantly effected by reconnection with targets. However, there are significant quantitatively and morphometrically assessable differences between the experimental groups depending on the tissue the RGCs are connected with visual targets. Regenerating RGCs show the highest stability in morphology if reconnected with visual target tissue.

CONCLUSIONS

Adult RGCs of the rat can be reconnected with visual centers using a peripheral nerve graft. This reconnection stabilizes the cells at morphological and the retina at functional levels for a long period of time, although it does not significantly increase cell survival.

摘要

目的

成年视网膜神经节细胞(RGCs)可以在用于替代远端视神经残端的周围神经移植物中再生其切断的轴突。我们通过引导其再生轴突进入不同的终末区来检查 RGCs 的长期稳定性。

方法

成年大鼠的视神经(ON)在眼眶内完全切断,其眼端与不同的视觉靶区(皮质、中脑)或非视觉区(如肌肉)相连。对照组由盲端移植物和无移植物的 ON 切断组成。定期通过视网膜电图检查视网膜功能。术后 1、6 和 9 个月,用 4-(4-(二癸基氨基)-苯乙烯基)-N-甲基吡啶鎓碘化物逆行标记 RGCs,并进行形态计量学检查。再生的 RGC 分为代表形态类型 I、II 和 III 的三个主要类。

结果

我们的数据表明,尽管轴突数量很少,不到 1%,而且与靶组织的重新连接并没有显著影响,但在移植后长达 9 个月,再生的 RGC 在视神经上保持稳定。然而,根据 RGC 与视觉靶组织相连的组织,实验各组之间存在显著的定量和形态计量学可评估差异。如果与视觉靶组织重新连接,再生的 RGC 在形态上表现出最高的稳定性。

结论

大鼠的成年 RGC 可以使用周围神经移植物与视觉中枢重新连接。这种重新连接在很长一段时间内稳定了细胞在形态和视网膜在功能水平上的状态,尽管它并没有显著增加细胞的存活率。

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