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Activating Transcription Factor 3 a Useful Marker for Regenerative Response after Nerve Root Injury

机译:激活转录因子3神经根损伤后再生反应的有用标记。

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摘要

Activating transcription factor 3 (ATF3) is induced in various tissues in response to stress. In this experiment, ATF3 expression was studied in adult rats subjected either to a dorsal or ventral root avulsion (VRA; L4-6), or sciatic nerve transection (SNT). Post-operative survival times varied between 1.5 h and 3 weeks. In additional experiments an avulsed ventral root was directly replanted to the spinal cord. Dorsal root ganglias (DRGs) from humans exposed to traumatic dorsal root avulsions were also examined. After SNT ATF3 immunoreactivity (ATF3 IR) was detected in a few DRG neurons already 6 h after the lesion. After 24 h the number had clearly increased and still at 3 weeks DRG neurons remained labeled. In the ventral horn, ATF3 IR in motoneurons (MN) was first detected 24 h after the SNT, and still 3 weeks post-operatively lesioned MN showed ATF3 labeling. After a VRA many spinal MN showed ATF3 IR already after 3 h, and after 6 h all MN were labeled. At 3 weeks a majority of the lesioned MN had died, but all the remaining ones were labeled. When an avulsed ventral root was directly replanted, MN survived and were still labeled at 5 weeks. In DRG, a few neurons were labeled already at 1.5 h after a dorsal root avulsion. At 24 h the number had increased but still only a minority of the neurons were labeled. At 3 days the number of labeled neurons was reduced, and a further reduction was at hand at 7 days and 3 weeks. In parallel, in humans, 3 days after a traumatic dorsal root avulsion, only a few DRG neurons showed ATF3 IR. At 6 weeks no labeled neurons could be detected. These facts imply that ATF3 response to axotomy involves a distance-dependent mechanism. ATF3 also appears to be a useful and reliable neuronal marker of nerve lesions even in humans. In addition, ATF3 up-regulation in both motor and sensory neurons seems to be linked to regenerative competence.
机译:响应压力,在各种组织中诱导激活转录因子3(ATF3)。在该实验中,在成年大鼠的背侧或腹侧根部撕脱(VRA; L4-6)或坐骨神经横切(SNT)中研究了ATF3的表达。术后生存时间在1.5周至3周之间不等。在其他实验中,撕脱的腹侧根直接植入到脊髓中。还检查了暴露于创伤性背根撕脱的人的背根神经节(DRG)。 SNT后,在病变后6h的一些DRG神经元中检测到了免疫反应性(ATF3 IR)。在24小时后,该数目明显增加,并且仍然在3周时仍标记了DRG神经元。在腹角,首先在SNT后24 h检测到运动神经元(MN)中的ATF3 IR,并且在病变后3周仍显示有ATF3标记。在进行VRA后,许多脊髓MN在3 h后已经显示ATF3 IR,而在6 h之后,所有MN都被标记了。在3周时,大部分病变MN死亡,但其余所有MN均已贴上标签。当直接撕下腹侧根后,MN存活下来,并在5周时仍贴上标签。在DRG中,背根撕脱术后1.5 h已经标记了一些神经元。在24小时时,该数目增加了,但仍然只有少数神经元被标记。在第3天时,标记神经元的数量减少了,在第7天和第3周时进一步减少了。同时,在人类中,背侧根部撕脱伤后3天,只有少数DRG神经元显示ATF3 IR。在6周时,未检测到标记的神经元。这些事实暗示ATF3对轴切术的反应涉及距离依赖性机制。即使在人类中,ATF3也似乎是神经病变的有用且可靠的神经元标记。此外,运动和感觉神经元中的ATF3上调似乎与再生能力有关。

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