A targeted extracellular vesicles loaded with montelukast in the treatment of demyelinating diseases

髓鞘 多发性硬化 少突胶质细胞 孟鲁卡斯特 体内 再髓鞘化 微泡 癌症研究 病变 免疫学 医学 脱髓鞘病 生物 神经科学 中枢神经系统 病理 小RNA 生物化学 生物技术 哮喘 基因
作者
Yun Xiao,Yuan Zhang,Yuhan Gao,Zhuo-Hua Zhao,Jin He,Rui Gao,Yuxin Guo,Libin Wang,Xing Li
出处
期刊:Biochemical and Biophysical Research Communications [Elsevier BV]
卷期号:594: 31-37 被引量:18
标识
DOI:10.1016/j.bbrc.2022.01.051
摘要

The main pathological characteristics of demyelinating diseases are central nervous system (CNS) myelin damage, and the differentiation of oligodendrocyte precursor cells is the therapeutic target of myelin repair. Previous studies have found that a large number of platelet-derived growth factor receptor α(PDGFRα) positive oligodendrocyte progenitor cells (OPCs) accumulate in the lesion area of myelin injury, and differentiation is blocked. However, the therapeutic effects of drugs currently used clinically on OPCs differentiation and myelin repair are limited. The main reason is that it is difficult to reach the effective concentration of the drug in the lesion area. Therefore, efficiently delivering into the CNS lesion area is of great significance for the treatment of MS. Natural exosomes have good biocompatibility and are ideal drug carriers. The delivery of drugs to lesion areas can be achieved by giving the exosomes armed targeting ligand. Therefore, in this study, combining exosomes with PDGFA helps them accumulate in OPCs in vitro and in vivo . Further, load montelukast into exosomes to achieve targeted therapy for cuprizone-induced demyelination animal model. The implementation of this research will help provide effective treatments for demyelinating diseases and lay a theoretical foundation for its application in the clinical treatment of different demyelinating diseases. • OPC surface receptor PDGFRα is a potential target for drug delivery in demyelinating diseases. • The ligand-modified exosomes dramatically increased targeting efficiency to the oligodendrocyte lineages in vitro and in vivo. • EVPs-montelukast exerts the therapeutic ability in the demyelination animal and promotes myelin regeneration.

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