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负载肝X受体激动剂的高密度脂蛋白纳米盘可减轻小鼠胶质瘤模型的肿瘤负担并介导长期存活

HDL Nanodiscs Loaded with Liver X Receptor Agonist Decreases Tumor Burden and Mediates Long-term Survival in Mouse Glioma Model.

作者信息

Halseth Troy A, Mujeeb Anzar A, Liu Lisha, Banerjee Kaushik, Lang Nigel, Hollon Todd, Yu Minzhi, Roest Mark Vander, Mei Ling, He Hongliang, Sheth Maya, Castro Maria G, Schwendeman Anna

出版信息

bioRxiv. 2025 Apr 3:2025.04.01.646644. doi: 10.1101/2025.04.01.646644.

Abstract

Glioblastoma multiforme (GBM) is highly aggressive primary brain tumor with a 5-year survival rate of 7%. Previous studies have shown that GBM tumors have a reduced capacity to produce cholesterol and instead depend on the uptake of cholesterol produced by astrocytes. To target cholesterol metabolism to induce cancer cell death, synthetic high-density lipoprotein (sHDL) nanodiscs delivering Liver-X-Receptor (LXR) agonists and CpG oligonucleotides for targeting GBM were investigated. LXR agonists synergize with sHDL nanodiscs by increasing the expression of the ABCA1 cholesterol CpG oligonucleotides are established adjuvants used in cancer immunotherapy that work through the toll-like receptor 9 pathway. In the present study, treatment with GW-CpG-sHDL nanodiscs increased the expression of cholesterol efflux transporters on murine GL261 cells leading to enhanced cholesterol removal. Experiments in GL261-tumor-bearing mice revealed combining GW-CpG-sHDL nanodiscs with radiation (IR) therapy significantly increases median survival compared to GW-CpG-sHDL or IR alone. Furthermore, 66% of long-term survivors from the GW-CpG-sHDL +IR treatment group showed no tumor tissue when rechallenged.

摘要

多形性胶质母细胞瘤(GBM)是一种极具侵袭性的原发性脑肿瘤,5年生存率为7%。先前的研究表明,GBM肿瘤产生胆固醇的能力降低,转而依赖于摄取星形胶质细胞产生的胆固醇。为了靶向胆固醇代谢以诱导癌细胞死亡,研究了用于靶向GBM的递送肝X受体(LXR)激动剂和CpG寡核苷酸的合成高密度脂蛋白(sHDL)纳米盘。LXR激动剂通过增加ABCA1胆固醇的表达与sHDL纳米盘协同作用,CpG寡核苷酸是用于癌症免疫治疗的既定佐剂,通过Toll样受体9途径发挥作用。在本研究中,用GW-CpG-sHDL纳米盘处理增加了小鼠GL261细胞上胆固醇流出转运蛋白的表达,导致胆固醇清除增强。在携带GL261肿瘤的小鼠中进行的实验表明,与单独使用GW-CpG-sHDL或放疗(IR)相比,将GW-CpG-sHDL纳米盘与放疗(IR)联合使用可显著提高中位生存期。此外,GW-CpG-sHDL +IR治疗组66%的长期存活者再次受到挑战时未显示肿瘤组织。

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