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首页> 外文期刊>Neural development >Genome-wide expression profile of the response to spinal cord injury in Xenopus laevis reveals extensive differences between regenerative and non-regenerative stages
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Genome-wide expression profile of the response to spinal cord injury in Xenopus laevis reveals extensive differences between regenerative and non-regenerative stages

机译:非洲爪蟾对脊髓损伤反应的全基因组表达谱揭示了再生和非再生阶段之间的广泛差异

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Background Xenopus laevis has regenerative and non-regenerative stages. As a tadpole, it is fully capable of functional recovery after a spinal cord injury, while its juvenile form (froglet) loses this capability during metamorphosis. We envision that comparative studies between regenerative and non-regenerative stages in Xenopus could aid in understanding why spinal cord regeneration fails in human beings. Results To identify the mechanisms that allow the tadpole to regenerate and inhibit regeneration in the froglet, we obtained a transcriptome-wide profile of the response to spinal cord injury in Xenopus regenerative and non-regenerative stages. We found extensive transcriptome changes in regenerative tadpoles at 1 day after injury, while this was only observed by 6 days after injury in non-regenerative froglets. In addition, when comparing both stages, we found that they deployed a very different repertoire of transcripts, with more than 80% of them regulated in only one stage, including previously unannotated transcripts. This was supported by gene ontology enrichment analysis and validated by RT-qPCR, which showed that transcripts involved in metabolism, response to stress, cell cycle, development, immune response and inflammation, neurogenesis, and axonal regeneration were regulated differentially between regenerative and non-regenerative stages. Conclusions We identified differences in the timing of the transcriptional response and in the inventory of regulated transcripts and biological processes activated in response to spinal cord injury when comparing regenerative and non-regenerative stages. These genes and biological processes provide an entry point to understand why regeneration fails in mammals. Furthermore, our results introduce Xenopus laevis as a genetic model organism to study spinal cord regeneration.
机译:背景非洲爪蟾具有再生和非再生阶段。作为a,它完全能够在脊髓损伤后恢复功能,而其幼体(小蛙)在变态过程中会失去这种能力。我们设想,非洲爪蟾的再生阶段和非再生阶段之间的比较研究可以帮助理解为什么人类的脊髓再生失败。结果为了确定允许the再生并抑制蛙蛙再生的机制,我们获得了非洲爪蟾再生和非再生阶段对脊髓损伤反应的转录组范围的概况。我们发现,在受伤后1天,再生extensive的转录组发生了广泛的变化,而在非再生小青蛙中,只有在受伤后6天才观察到这一变化。此外,在比较两个阶段时,我们发现它们部署了非常不同的成绩单,其中80%以上的内容仅在一个阶段受到监管,包括以前未注释的成绩单。这得到了基因本体论富集分析的支持,并通过RT-qPCR进行了验证,结果表明,参与代谢的转录本,对应激的应答,细胞周期,发育,免疫应答和炎症,神经发生和轴突再生的调节都与非再生阶段。结论我们在比较再生阶段和非再生阶段时,发现了转录反应的时机以及调节的转录本和因脊髓损伤而激活的生物过程的库存差异。这些基因和生物学过程为了解为什么哺乳动物再生失败提供了切入点。此外,我们的研究结果将非洲爪蟾作为遗传模型生物来研究脊髓再生。

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