Auto-loaded TRAIL-exosomes derived from induced neural stem cells for brain cancer therapy

癌症研究 体内 癌症 神经干细胞 重编程 微泡 癌细胞 离体 脑瘤 生物 医学 干细胞 病理 细胞 细胞生物学 小RNA 内科学 基因 生物化学 生物技术
作者
Xiaopei Zhang,Hannah Taylor,Alain Valdivia,Rajaneekar Dasari,A. G. Buckley,Emily E. Bonacquisti,Juliane Nguyen,Krishna Kanchi,David L. Corcoran,Laura E. Herring,Dennis A. Steindler,Albert S. Baldwin,Shawn Hingtgen,Andrew Satterlee
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:372: 433-445 被引量:3
标识
DOI:10.1016/j.jconrel.2024.06.048
摘要

Transdifferentiation (TD), a somatic cell reprogramming process that eliminates pluripotent intermediates, creates cells that are ideal for personalized anti-cancer therapy. Here, we provide the first evidence that extracellular vesicles (EVs) from TD-derived induced neural stem cells (Exo-iNSCs) are an efficacious treatment strategy for brain cancer. We found that genetically engineered iNSCs generated EVs loaded with the tumoricidal gene product TRAIL at nearly twice the rate of their parental fibroblasts, and TRAIL produced by iNSCs was naturally loaded into the lumen of EVs and arrayed across their outer membrane (Exo-iNSC-TRAIL). Uptake studies in ex vivo organotypic brain slice cultures showed that Exo-iNSC-TRAIL selectively accumulates within tumor foci, and co-culture assays demonstrated that Exo-iNSC-TRAIL killed metastatic and primary brain cancer cells more effectively than free TRAIL. In an orthotopic mouse model of brain cancer, Exo-iNSC-TRAIL reduced breast-to-brain tumor xenografts by approximately 3000-fold compared to treatment with free TRAIL, with all Exo-iNSC-TRAIL treated animals surviving through 90 days post-treatment. In additional in vivo testing against aggressive U87 and invasive GBM8 glioblastoma tumors, Exo-iNSC-TRAIL also induced a statistically significant increase in survival. These studies establish a novel, easily generated, stable, tumor-targeted EV to efficaciously treat multiple forms of brain cancer.
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