Targeted liposomes for combined delivery of artesunate and temozolomide to resistant glioblastoma

替莫唑胺 药理学 体内 纳米载体 血脑屏障 脂质体 医学 药物输送 胶质瘤 跨细胞 癌症研究 联合疗法 药品 材料科学 生物 内科学 受体 纳米技术 内吞作用 生物技术 中枢神经系统
作者
Muhammad Ismail,Wen Yang,Yanfei Li,Tianran Chai,Dongya Zhang,Qiuli Du,Pir Muhammad,Sumaira Hanif,Meng Zheng,Yan Zou
出处
期刊:Biomaterials [Elsevier]
卷期号:287: 121608-121608 被引量:37
标识
DOI:10.1016/j.biomaterials.2022.121608
摘要

The effective treatment of glioblastoma (GBM) is a great challenge because of the blood-brain barrier (BBB) and the growing resistance to single-agent therapeutics. Targeted combined co-delivery of drugs could circumvent these challenges; however, the absence of more effective combination drug delivery strategies presents a potent barrier. Here, a unique combination ApoE-functionalized liposomal nanoplatform based on artesunate-phosphatidylcholine (ARTPC) encapsulated with temozolomide (ApoE-ARTPC@TMZ) was presented that can successfully co-deliver dual therapeutic agents to TMZ-resistant U251-TR GBM in vivo. Examination in vitro showed ART-mediated inhibition of DNA repair through the Wnt/β-catenin signaling cascade, which also improved GBM sensitivity to TMZ, resulting in enhanced synergistic DNA damage and induction of apoptosis. In assessing BBB permeation, the targeted liposomes were able to effectively traverse the BBB through low-density lipoprotein family receptors (LDLRs)-mediated transcytosis and achieved deep intracranial tumor penetration. More importantly, the targeted combination liposomes resulted in a significant decrease of U251-TR glioma burden in vivo that, in concert, substantially improved the survival of mice. Additionally, by lowering the effective dosage of TMZ, the combination liposomes reduced systemic TMZ-induced toxicity, highlighting the preclinical potential of this novel integrative strategy to deliver combination therapies to brain tumors.
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