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基于氧化还原敏感透明质酸-ss-姜黄素胶束的双重靶向载体用于治疗脑胶质瘤的细胞摄取和生物分布研究。

Understanding the cellular uptake and biodistribution of a dual-targeting carrier based on redox-sensitive hyaluronic acid-ss-curcumin micelles for treating brain glioma.

机构信息

Department of Pharmaceutics, State Key Laboratory of Natural Medicines, China Pharmaceutical University, Nanjing 210009, PR China.

Faculty of Pharmaceutical Sciences, Government College University Faisalabad, Faisalabad, Pakistan.

出版信息

Int J Biol Macromol. 2019 Sep 1;136:143-153. doi: 10.1016/j.ijbiomac.2019.06.060. Epub 2019 Jun 11.

Abstract

The gliomas treatment is challenging due to the limits imposed by blood-brain barrier to the distribution of the drugs in the brain. Therefore, we designed a brain glioma targeting redox-sensitive hyaluronic acid (HA)-ss-curcumin (CUR) micelles. HA was conjugated to CUR through a disulfide bond, which could form micelles independently in aqueous solution. And we further increased the drug loading by loading free CUR. Brain penetration was achieved with Tween 80, whereas glioma-targeting was inclined by CD44-mediated endocytosis. Compared to the disulfide-free group, the redox-sensitive micelles exhibited rapid in vitro drug release under high glutathione conditions, significantly enhanced cell apoptosis and cellular uptake in G422 glioma cells. Redox-sensitive micelles displayed about 4.70-fold higher area under the curve in rats after intravenous injection in comparison to the free CUR and effectively accumulated in the brain. These findings suggest that redox-sensitive micelles could be a promising candidate to achieve brain targeted CUR delivery.

摘要

由于血脑屏障对药物在大脑中分布的限制,胶质瘤的治疗具有挑战性。因此,我们设计了一种针对脑胶质瘤的氧化还原敏感透明质酸(HA)-ss-姜黄素(CUR)胶束。HA 通过二硫键与 CUR 连接,在水溶液中可以独立形成胶束。并且我们通过装载游离 CUR 进一步增加了药物负载量。Tween 80 实现了脑穿透,而 CD44 介导的内吞作用则倾向于胶质瘤靶向。与不含二硫键的组相比,氧化还原敏感胶束在高谷胱甘肽条件下表现出快速的体外药物释放,显著增强了 G422 神经胶质瘤细胞的细胞凋亡和细胞摄取。与游离 CUR 相比,氧化还原敏感胶束在静脉注射后在大鼠体内的曲线下面积增加了约 4.70 倍,并且有效地在大脑中积累。这些发现表明,氧化还原敏感胶束可能是实现脑靶向 CUR 递送的有前途的候选物。

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