轴突
生物
再生(生物学)
轴突引导
神经科学
外囊肿
腹索神经
轴突丘
生长锥
神经系统
细胞生物学
解剖
蛋白质亚单位
遗传学
基因
作者
Christopher V. Gabel,Faustine Antoine,Chiou‐Fen Chuang,Aravinthan D. T. Samuel,Chieh Chang
出处
期刊:Development
[The Company of Biologists]
日期:2008-03-15
卷期号:135 (6): 1129-1136
被引量:97
摘要
The molecular and cellular mechanisms that allow adult-stage neurons to regenerate following damage are poorly understood. Recently, axons of motoneurons and mechanosensory neurons in adult C. elegans were found to regrow after being snipped by femtosecond laser ablation. Here, we explore the molecular determinants of adult-stage axon regeneration using the AVM mechanosensory neurons. The first step in AVM axon development is a pioneer axonal projection from the cell body to the ventral nerve cord. We show that regeneration of the AVM axon to the ventral nerve cord lacks the deterministic precision of initial axon development, requiring competition and pruning of unwanted axon branches. Nevertheless, axons of injured AVM neurons regrow to the ventral nerve cord with over 60% reliability in adult animals. In addition, in contrast to initial development, axon guidance during regeneration becomes heavily dependent on cytoplasmic protein MIG-10/Lamellipodin but independent of UNC-129/TGF-β repellent and UNC-40/DCC receptor, and axon growth during regeneration becomes heavily dependent on UNC-34/Ena and CED-10/Rac actin regulators. Thus, C. elegans may be used as a genetic system to characterize novel cellular and molecular mechanisms underlying adult-stage nervous system regeneration.
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