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An update on actively targeted liposomes in advanced drug delivery to glioma

胶质瘤 脂质体 药物输送 血脑屏障 医学 药理学 药品 癌症研究 毒品携带者 靶向给药 化学 内科学 中枢神经系统 生物化学 有机化学
作者
Solmaz Mojarad-Jabali,Masoud Farshbaf,Paul R. Walker,Salar Hemmati,Yousef Fatahi,Parvin Zakeri‐Milani,Muhammad Sarfraz,Hadi Valizadeh
出处
期刊:International Journal of Pharmaceutics [Elsevier]
卷期号:602: 120645-120645 被引量:80
标识
DOI:10.1016/j.ijpharm.2021.120645
摘要

High-grade glioma is one of the most aggressive types of cancer with a low survival rate ranging from 12 to 15 months after the first diagnosis. Though being the most common strategy for glioma therapy, conventional chemotherapy suffers providing the therapeutic dosage of common therapeutics mostly because of limited permeability of blood–brain barrier (BBB), and blood–brain tumor barrier (BBTB) to anticancer agents. Among various nanoformulations, liposomes are considered as the most popular carriers aimed for glioma therapy. However, non-targeted liposomes which passively accumulate in most of the cancer tissues mainly through the enhanced permeation and retention effect (EPR), may not be applicable for glioma therapy due to BBB tight junctions. In the recent decade, the surface modification of liposomes with different active targeting ligands has shown promising results by getting different chemotherapeutics across the BBB and BBTB and leading them into the glioma cells. The present review discusses the major barriers for drug delivery systems to glioma, elaborates the existing mechanisms for liposomes to traverse across the BBB, and explores the main strategies for incorporation of targeting ligands onto the liposomes. It subsequently investigates the most recent and relevant studies of actively targeted liposomes modified with antibodies, aptamers, monosaccharides, polysaccharides, proteins, and peptides applied for effective glioma therapy, and highlights the common challenges facing this area. Finally, the actively targeted liposomes undergoing preclinical and clinical studies for delivery of different anticancer agents to glioma cells will be reviewed.
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