Single-cell analysis of spinal cord injury reveals functional heterogeneity of oligodendrocyte lineage cells

少突胶质细胞 生物 髓鞘 细胞生物学 谱系(遗传) 脊髓损伤 神经科学 祖细胞 转录因子 脊髓 轴突 奥利格2 转录组 干细胞 中枢神经系统 基因表达 遗传学 基因
作者
Zexuan Wu,Guanglei Li,Kun Guo,Nan Zhang,Xuefeng Li,Fawang Zhang,Jianan Niu,Nanxiang Wang,Jianing Zu,Yufu Wang
出处
期刊:Gene [Elsevier BV]
卷期号:886: 147713-147713 被引量:1
标识
DOI:10.1016/j.gene.2023.147713
摘要

Spinal cord injury (SCI) is a traumatic condition that causes myelin destruction and neuronal death, making it challenging to reverse. In spinal cord tissue, oligodendrocyte progenitor cells and oligodendrocytes are essential for maintaining myelin morphology and axon regeneration. The decrease in oligodendrocyte lineage cells after SCI is a major factor contributing to the difficulty in restoring spinal cord function. However, there is still a lack of research on the status and intercellular communication between oligodendrocyte lineage cells after injury. The development of single-cell sequencing technology has enabled researchers to obtain highly accurate cellular transcriptional information, facilitating detailed studies of cellular subpopulations. This study delved into the cellular heterogeneity of oligodendrocyte lineage cells using a single-cell transcriptomic approach to uncover functional changes and cellular interactions during different time points after SCI. Our findings highlighted the critical roles of Psap (Prosaposin)/Gpr37l1 and Psap/Gpr37 ligand-receptor pairs among oligodendrocyte lineage cells. Furthermore, we predicted the transcription factors that may play a key regulatory role. We demonstrated for the first time that Junb acts almost exclusively in mature oligodendrocytes, which provides a potential target for the study of oligodendrocyte transcriptional mechanisms.
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