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合成引导通道释放的胶质细胞系源性神经营养因子促进大鼠面神经再生。

Glial cell line-derived neurotrophic factor released by synthetic guidance channels promotes facial nerve regeneration in the rat.

作者信息

Barras Florian M, Pasche Philippe, Bouche Nicolas, Aebischer Patrick, Zurn Anne D

机构信息

Department of ENT and Head and Neck Surgery, University Medical School, Lausanne, Switzerland.

出版信息

J Neurosci Res. 2002 Dec 15;70(6):746-55. doi: 10.1002/jnr.10434.

DOI:10.1002/jnr.10434
PMID:12444596
Abstract

Regeneration of the human facial nerve after lesion is often limited, leading to severe functional impairments, in particular when repair is delayed for several months, when cross-facial nerve grafts have to be performed, or in elderly patients. To improve the outcome, the potential accelerating and maturating effects of the neurotrophic factors glial cell line-derived neurotrophic factor (GDNF) and neurotrophin-3 (NT-3) on nerve regeneration were assessed using an axotomy model of the rat facial nerve. One-centimeter-long synthetic guidance channels releasing the neurotrophic factors over several weeks were used to bridge an 8 mm nerve gap, a distance that does not allow regeneration in the absence of growth factors. Nerve cables regenerated in the presence of GDNF showed a large number of myelinated axons 6 weeks after grafting (871 +/- 373, n = 5), whereas only 106 +/- 86 (n = 5) myelinated axons were counted in the presence of NT-3. Retrograde labeling with fluorogold revealed 981 +/- 450 (n = 5) and 53 +/- 38 (n = 5) retrogradely labeled motoneurons in the facial nucleus in the presence of GDNF and NT-3, respectively. No regenerated axons or retrogradely labeled cells were observed in the absence of growth factors (n = 6). These results demonstrate that GDNF, as previously described for the sciatic nerve, a mixed sensory and motor nerve, is also very efficient in promoting regeneration of the facial nerve, an essentially pure motor nerve. GDNF may therefore be useful in improving facial nerve regeneration in the clinic.

摘要

人类面神经损伤后的再生通常很有限,会导致严重的功能障碍,特别是在修复延迟数月、需要进行跨面神经移植时,或者在老年患者中。为了改善治疗效果,利用大鼠面神经轴突切断模型评估了神经营养因子胶质细胞源性神经营养因子(GDNF)和神经营养素-3(NT-3)对神经再生的潜在促进和成熟作用。使用能在数周内释放神经营养因子的1厘米长合成引导通道来桥接8毫米的神经间隙,在没有生长因子的情况下,这个距离无法实现再生。在GDNF存在的情况下再生的神经束在移植6周后显示出大量有髓轴突(871±373,n = 5),而在NT-3存在的情况下仅计数到106±86(n = 5)条有髓轴突。用荧光金逆行标记显示,在GDNF和NT-3存在的情况下,面神经核中分别有981±450(n = 5)和53±38(n = 5)个逆行标记的运动神经元。在没有生长因子的情况下未观察到再生轴突或逆行标记的细胞(n = 6)。这些结果表明,如先前在坐骨神经(一种混合感觉和运动神经)中所描述的,GDNF在促进面神经(一种基本纯运动神经)的再生方面也非常有效。因此,GDNF可能有助于改善临床上的面神经再生。

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