外体
体内
脊髓损伤
微泡
免疫疗法
小胶质细胞
炎症
神经保护
细胞生物学
癌症研究
化学
材料科学
免疫系统
药理学
医学
免疫学
脊髓
生物
生物化学
小RNA
神经科学
生物技术
基因
作者
Lu Bai,Jinpeng Gao,Peng Zhang,Sen Lin,Chuanjie Zhang
标识
DOI:10.1016/j.intimp.2024.111983
摘要
Developing biomimetic nanoparticles without off-target side-effects remains a major challenge in spinal cord injury (SCI) immunotherapy. In this paper, we have conducted a drug carrier which is biocompatible macrophages-exocytosed exosome-biomimetic manganese (Mn)-iron prussian blue analogues (MPBs) for SCI immunotherapy. Exosome-sheathed MPBs (E-MPBs) exhibit promoted microglia accumulation, alleviation from H2O2-induced microenvironment and inhibition of apoptosis and inflammation in vitro. In addition, E-MPBs possessed significant tissue repair and neuroprotection in vivo. These properties endowed E-MPBs with great improvement in vivo in function recovery, resulting in anti-neuroinflammation activity and excellent biocompatibility in mice SCI model. As a promising treatment for efficient SCI immunotherapy, these results demonstrate the use of exosome-sheathed biomimetic nanoparticles exocytosed by anti-inflammation cells is feasible.
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