白细胞介素-3调节巨噬细胞吞噬活性并促进脊髓损伤修复。

Interleukin-3 Modulates Macrophage Phagocytic Activity and Promotes Spinal Cord Injury Repair.

作者信息

Li Jianjian, Zheng Meige, Ouyang Fangru, Ye Jianan, Huang Jinxin, Zhao Yuanzhe, Wang Jingwen, Shan Fangli, Li Ziyu, Yu Shuishen, Yao Fei, Tian Dasheng, Cheng Li, Jing Juehua

机构信息

Department of Orthopaedics, The Second Affiliated Hospital of Anhui Medical University, Hefei, China.

Institute of Orthopaedics, Research Center for Translational Medicine, The Second Affiliated Hospital of Anhui Medical University, Hefei, China.

出版信息

CNS Neurosci Ther. 2024 Dec;30(12):e70181. doi: 10.1111/cns.70181.

DOI:10.1111/cns.70181

PMID:39697159

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11656101/

Abstract

BACKGROUND

Effective clearance of lipid-rich debris by macrophages is critical for neural repair and regeneration after spinal cord injury (SCI). Interleukin-3 (IL-3) has been implicated in programming microglia to cluster and clear pathological aggregates in neurodegenerative disease. Yet, the influence of IL-3 on lipid debris clearance post-SCI is not well characterized.

METHODS

We established a mouse model of spinal cord compression injury to investigate the role of IL-3. Blockage of IL-3 was achieved through intrathecal delivery of an IL-3-neutralizing antibody, while IL-3 activation was augmented via in situ injection of recombinant IL-3 into the lesion site immediately post-SCI. Immunofluorescence staining was performed to determine IL-3 and IL-3Rα sources and distribution, lipid droplet accumulation, neuron preservation, and axon regeneration after SCI. The Basso Mouse Scale (BMS) and footprint analysis were employed to evaluate locomotor function recovery.

RESULTS

We found that IL-3 expression was significantly upregulated post-SCI, peaking at 14 days post-injury (dpi) and persisting until 28 dpi. Notably, IL-3 was primarily secreted by astrocytes surrounding the lesion epicenter. Correspondingly, IL-3Rα was predominantly observed in macrophages within the injury core, also elevating at 14 dpi. Neutralization of IL-3 led to increased lipid droplet accumulation, along with markedly widespread of macrophages and decreased neuronal survival, resulting in severe motor deficits compared to controls. Conversely, in situ injection of IL-3 reduced lipid droplet accumulation in macrophages, preserved neurons, promoted axon regeneration, and ultimately contributed to the recovery of motor function after SCI.

CONCLUSION

Our findings shed light on the role of IL-3 in modulating macrophage phagocytic activity and suggest that the IL-3/IL-3Rα pathway may be a potential therapeutic target for enhancing neural repair and functional recovery after SCI.

摘要

背景

巨噬细胞有效清除富含脂质的碎片对于脊髓损伤（SCI）后的神经修复和再生至关重要。白细胞介素-3（IL-3）与神经退行性疾病中促使小胶质细胞聚集并清除病理聚集体有关。然而，IL-3对SCI后脂质碎片清除的影响尚未得到充分阐明。

方法

我们建立了脊髓压迫损伤小鼠模型来研究IL-3的作用。通过鞘内注射IL-3中和抗体来阻断IL-3，而在SCI后立即将重组IL-3原位注射到损伤部位以增强IL-3的活性。进行免疫荧光染色以确定SCI后IL-3和IL-3Rα的来源及分布、脂滴积累、神经元保存和轴突再生情况。采用巴索小鼠量表（BMS）和足迹分析来评估运动功能恢复情况。

结果

我们发现SCI后IL-3表达显著上调，在损伤后14天（dpi）达到峰值，并持续至28 dpi。值得注意的是，IL-3主要由损伤震中周围的星形胶质细胞分泌。相应地，IL-3Rα主要在损伤核心内的巨噬细胞中观察到，在14 dpi时也有所升高。中和IL-3导致脂滴积累增加，同时巨噬细胞明显广泛分布，神经元存活率降低，与对照组相比导致严重的运动功能缺陷。相反，原位注射IL-3减少了巨噬细胞中的脂滴积累，保存了神经元，促进了轴突再生，并最终有助于SCI后运动功能的恢复。