首页> 美国卫生研究院文献>Wiley-Blackwell Online Open >Peripheral Facial Nerve Axotomy in Mice Causes Sprouting of Motor Axons Into Perineuronal Central White Matter: Time Course and Molecular Characterization
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Peripheral Facial Nerve Axotomy in Mice Causes Sprouting of Motor Axons Into Perineuronal Central White Matter: Time Course and Molecular Characterization

机译:小鼠周围性面神经轴索切开术导致运动轴突发芽到神经周围中央白色物质:时间过程和分子表征。

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摘要

Generation of new axonal sprouts plays an important role in neural repair. In the current study, we examined the appearance, composition and effects of gene deletions on intrabrainstem sprouts following peripheral facial nerve axotomy. Axotomy was followed by the appearance of galanin+ and calcitonin gene-related peptide (CGRP)+ sprouts peaking at day 14, matching both large, neuropeptide+ subpopulations of axotomized facial motoneurons, but with CGRP+ sprouts considerably rarer. Strong immunoreactivity for vesicular acetylcholine transporter (VAChT) and retrogradely transported MiniRuby following its application on freshly cut proximal facial nerve stump confirmed their axotomized motoneuron origin; the sprouts expressed CD44 and alpha7beta1 integrin adhesion molecules and grew apparently unhindered along neighboring central white matter tracts. Quantification of the galanin+ sprouts revealed a stronger response following cut compared with crush (day 7–14) as well as enhanced sprouting after recut (day 8 + 6 vs. 14; 14 + 8 vs. 22), arguing against delayed appearance of sprouting being the result of the initial phase of reinnervation. Sprouting was strongly diminished in brain Jun-deficient mice but enhanced in alpha7 null animals that showed apparently compensatory up-regulation in beta1, suggesting important regulatory roles for transcription factors and the sprout-associated adhesion molecules. Analysis of inflammatory stimuli revealed a 50% reduction 12–48 hours following systemic endotoxin associated with neural inflammation and a tendency toward more sprouts in TNFR1/2 null mutants (P = 10%) with a reduced inflammatory response, indicating detrimental effects of excessive inflammation. Moreover, the study points to the usefulness of the facial axotomy model in exploring physiological and molecular stimuli regulating central sprouting. J. Comp. Neurol. 518:699–721, 2010. © 2009 Wiley-Liss, Inc.
机译:轴突新芽的产生在神经修复中起重要作用。在当前的研究中,我们检查了周围面神经轴突切开后脑干内芽的基因缺失的外观,组成和影响。切开后,出现甘丙肽 + 和降钙素基因相关肽(CGRP) + 发芽,在第14天达到峰值,与大的神经肽 + 轴突切除的运动神经元的亚群,但是带有CGRP + 的豆芽相当少见。对囊泡乙酰胆碱转运蛋白(VAChT)和逆行转运的MiniRuby的强烈免疫反应性,将其应用于刚切下的近端面神经残端,证实了它们是轴突化的运动神经元。芽苗表达CD44和alpha7beta1整合素粘附分子,并沿相邻的中央白质束不受阻碍地生长。甘丙肽 + 芽的定量显示,切碎后的压榨响应比压榨(第7-14天)强,重切后的发芽增强(第8 + 6对14天; 14 + 8对22天) ),反对将发芽的延迟外观归因于重新神经化的初始阶段。在脑Jun缺乏的小鼠中发芽明显减少,但在alpha7无动物中增强了发芽,后者在beta1中表现出明显的补偿性上调,表明转录因子和与芽相关的粘附分子具有重要的调节作用。对炎症刺激的分析显示,与神经炎症相关的系统内毒素后12-48小时减少了50%,TNFR1 / 2空突变体(P = 10%)中发芽的趋势更多,炎症反应减少,表明过度炎症的有害影响。此外,研究指出了面部轴突切开术模型在探索调节中央发芽的生理和分子刺激中的有用性。 J.比较神经元。 518:699–721,2010年。©2009 Wiley-Liss,Inc.

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