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脊髓损伤后髓磷脂碎片的产生与清除

Generation and clearance of myelin debris after spinal cord injury.

作者信息

Li Chaoyuan, Luo Wenqi, Hussain Irshad, Niu Renrui, He Xiaodong, Xiang Chunyu, Guo Fengshuo, Liu Wanguo, Gu Rui

机构信息

Department of Orthopedic Surgery, China-Japan Union Hospital, Jilin University, Changchun, Jilin Province, China.

Department of Chemistry and Chemical Engineering, SBA School of Science & Engineering, Lahore University of Management Sciences, DHA, Lahore, Pakistan.

出版信息

Neural Regen Res. 2026 Apr 1;21(4):1512-1527. doi: 10.4103/NRR.NRR-D-24-01405. Epub 2025 Apr 29.

Abstract

Traumatic spinal cord injury often leads to the disintegration of nerve cells and axons, resulting in a substantial accumulation of myelin debris that can persist for years. The abnormal buildup of myelin debris at sites of injury greatly impedes nerve regeneration, making the clearance of debris within these microenvironments crucial for effective post-spinal cord injury repair. In this review, we comprehensively outline the mechanisms that promote the clearance of myelin debris and myelin metabolism and summarize their roles in spinal cord injury. First, we describe the composition and characteristics of myelin debris and explain its effects on the injury site. Next, we introduce the phagocytic cells involved in myelin debris clearance, including professional phagocytes (macrophages and microglia) and non-professional phagocytes (astrocytes and microvascular endothelial cells), as well as other cells that are also proposed to participate in phagocytosis. Finally, we focus on the pathways and associated targets that enhance myelin debris clearance by phagocytes and promote lipid metabolism following spinal cord injury. Our analysis indicates that myelin debris phagocytosis is not limited to monocyte-derived macrophages, but also involves microglia, astrocytes, and microvascular endothelial cells. By modulating the expression of genes related to phagocytosis and lipid metabolism, it is possible to modulate lipid metabolism disorders and influence inflammatory phenotypes, ultimately affecting the recovery of motor function following spinal cord injury. Additionally, therapies such as targeted mitochondrial transplantation in phagocytic cells, exosome therapy, and repeated trans-spinal magnetic stimulation can effectively enhance the removal of myelin debris, presenting promising potential for future applications.

摘要

创伤性脊髓损伤常导致神经细胞和轴突解体,致使髓磷脂碎片大量堆积,且这种堆积可能持续数年。损伤部位髓磷脂碎片的异常堆积严重阻碍神经再生,因此清除这些微环境中的碎片对于脊髓损伤后的有效修复至关重要。在本综述中,我们全面概述了促进髓磷脂碎片清除和髓磷脂代谢的机制,并总结了它们在脊髓损伤中的作用。首先,我们描述了髓磷脂碎片的组成和特征,并解释了其对损伤部位的影响。接下来,我们介绍参与髓磷脂碎片清除的吞噬细胞,包括专业吞噬细胞(巨噬细胞和小胶质细胞)和非专业吞噬细胞(星形胶质细胞和微血管内皮细胞),以及其他也被认为参与吞噬作用的细胞。最后,我们重点关注增强吞噬细胞清除髓磷脂碎片并促进脊髓损伤后脂质代谢的途径和相关靶点。我们的分析表明,髓磷脂碎片吞噬作用不仅限于单核细胞衍生的巨噬细胞,还涉及小胶质细胞、星形胶质细胞和微血管内皮细胞。通过调节与吞噬作用和脂质代谢相关的基因表达,有可能调节脂质代谢紊乱并影响炎症表型,最终影响脊髓损伤后运动功能的恢复。此外,诸如在吞噬细胞中进行靶向线粒体移植、外泌体疗法和重复经脊髓磁刺激等治疗方法可以有效增强髓磷脂碎片的清除,展现出未来应用的广阔前景。

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