The outgrowth response of the axons of developing and regenerating rat retinal ganglion cells in vitro to neurotrophin treatment.

Ovokeloye Avwenagha, Gregor Campbell, Margaret M Bird
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引用次数: 19

Abstract

BDNF and NT-4 (but not NT-3 or CNTF) significantly enhanced the outgrowth of early embryonic and adult regenerating RGC axons when provided with a supportive substrate in vitro. BDNF and NT-4 treatment transiently increased RGC axon outgrowth from E15 rat retinas but not from retinas at older embryonic ages. The transient effect of BDNF and NT-4 and the inability of the neurotrophins to promote outgrowth from older embryonic retinal explants suggests a time frame of neurotrophin action and that other chemical factors (target-derived or otherwise) may be necessary for the continued maintenance of developing RGC axons. BDNF and NT-4 also enhanced the outgrowth of regenerating axons from adult retinal explants, but appeared to have a more subtle effect on axon outgrowth, in that the growth-promoting effects of BDNF and NT-4 appeared continuous throughout the incubation period. The suppression of RGC axon outgrowth from embryonic and adult retinae cultured in trkB-IgG-containing medium suggests that the response of developing and regenerating axons, to BDNF and NT-4 are likely to occur through trkB signalling.

发育和再生大鼠视网膜神经节细胞轴突对神经营养因子的体外生长反应。
BDNF和NT-4(而不是NT-3或CNTF)在体外提供支持底物时显著促进早期胚胎和成年再生RGC轴突的生长。BDNF和NT-4处理短暂地增加了E15大鼠视网膜的RGC轴突生长,但在胚胎年龄较大的视网膜上没有。BDNF和NT-4的短暂作用以及神经营养因子无法促进老年胚胎视网膜外植体的生长表明,神经营养因子的作用有一个时间框架,其他化学因子(靶源性或其他)可能是继续维持RGC轴突发育所必需的。BDNF和NT-4也促进了成人视网膜外植体再生轴突的生长,但对轴突生长的影响似乎更为微妙,因为在整个培养期间,BDNF和NT-4的生长促进作用持续存在。在含有trkB- igg的培养基中培养的胚胎和成人视网膜的RGC轴突生长受到抑制,这表明轴突的发育和再生对BDNF和NT-4的反应可能是通过trkB信号传导发生的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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