| Literature DB >> 30346089 |
Wenbo Qian1, Min Qian2, Yi Wang3, Jianfei Huang4, Jian Chen1, Lanchun Ni1, Qingfeng Huang1, Qianqian Liu1, Peipei Gong1, Shiqiang Hou1, Hui Zhu5, Zhongzheng Jia6, Dandan Shen6, Changlai Zhu7, Rui Jiang1, Junlong Sun1, Junzhong Yao1, Zhongyu Tang1, Xiang Ji1, Jinlong Shi1, Rongqin Huang2, Wei Shi1.
Abstract
Accumulating studies have investigated the efficacy of receptor-mediated delivery of hydrophobic drugs in glioma chemotherapy. Here, a delivery vehicle comprising polyethylene glycol (PEG) and oxidized nanocrystalline mesoporous carbon particles (OMCN) linked to the Pep22 polypeptide targeting the low-density lipoprotein receptor (LDLR) is designed to generate a novel drug-loaded system, designated as OMCN-PEG-Pep22/DOX (OPPD). This system effectively targets glioma cells and the blood-brain barrier and exerts therapeutic efficacy through both near-infrared (NIR) photothermal and chemotherapeutic effects of loaded doxycycline (DOX). Pathological tissue microarrays show an association of LDLR overexpression in human glioma tissue with patient survival.NIR irradiation treatment and magnetic resonance imaging results show that OPPD reaches the effective glioma-killing temperature in a glioma-bearing rat with a skull bone removal model and considerably reduces glioma sizes relative to the drug-loaded system without the Pep22 peptide modification and the control respectively. Thus, OPPD not only effectively targets LDLR-overexpressing glioma but also exerts a dual therapeutic effect by transporting DOX into the glioma and generating thermal effects with near-infrared irradiation to kill tumor cells. These collective findings support the utility of the novel OPPD drug-loaded system as a promising drug delivery vehicle for clinical application in glioma therapy.Entities:
Keywords: LDLR; dual targeting; glioma treatment; nanoparticle design; thermal therapy
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Year: 2018 PMID: 30346089 DOI: 10.1002/smll.201801905
Source DB: PubMed Journal: Small ISSN: 1613-6810 Impact factor: 13.281