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Dissecting the Molecular Signature of Spinal Cord Regeneration in the Axolotl Model

机译:解剖腋下模型中脊髓再生的分子特征

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Thousands of people are affected by central nervous system (CNS) dysfunctions each year, with stroke and spinal cord injury (SCI) being the most frequent causes. Although there is some evidence of partial CNS self-repair (via migration of neural stem cells to the injury zone and adult neurogenesis), due to restricted regeneration capacity in mammals, acute or chronic spinal cord injuries cannot be repaired completely. Therefore, to expand the availability of treatment options for SCI, research on highly regenerative animals has become essential. Among vertebrates, axolotl, a salamander species, has been emerging as a powerful model to explore the molecular mechanisms of regeneration due to its exceptional regenerative capacity. In this study, gene expression modulation for regenerative-capable neotenic axolotl during spinal cord regeneration has been investigated. Next-generation sequencing was applied for the collected regeneration samples at zero and seven days post-amputation (dpa). The data obtained from the analyzed samples revealed 363 genes differentially expressed, mostly downregulated, between zero dpa and seven?dpa. The extracellular matrix, cell-cell adhesion, and immune system-related processes and pathways were enriched by gene ontology and the Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analyses. Based on these data, we conclude that the downregulation of immune system-related biological processes is crucial for spinal cord regeneration.
机译:成千上万的人受到中枢神经系统(CNS)每年功能障碍的影响,中风和脊髓损伤(SCI)是最常见的原因。尽管存在部分CNS自我修复的证据(通过神经干细胞迁移到损伤区和成人神经发生),因此由于哺乳动物的限制性再生能力,急性或慢性脊髓损伤不能完全修复。因此,为了扩大SCI的治疗方案的可用性,对高度再生动物的研究变得必不可少。在脊椎动物中,Axolotl,蝾螈物种,已经成为一种强大的模型,以探讨其特殊的再生能力导致的再生的分子机制。在该研究中,研究了在脊髓再生过程中进行再生能力的新甲氧运动的基因表达调制。将收集的再生样品施加下一代测序,截止截肢后零和七天(DPA)。从分析的样品获得的数据显示差异表达363个基因,大多下调,零DPA和七个dPA之间。细胞外基质,细胞 - 细胞粘附和免疫系统相关方法和途径通过基因本体和基因和基因组(Kegg)途径富集分析进行富集。基于这些数据,我们得出结论,免疫系统相关的生物过程的下调对于脊髓再生至关重要。

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