通过基于铁死亡的治疗,用苯硼酸修饰的 PLGA 纳米粒递呈协同药物组合来增强抗癌潜能。
Enhancing anti-cancer potential by delivering synergistic drug combinations via phenylboronic acid modified PLGA nanoparticles through ferroptosis-based therapy.
机构信息
Centre for Pharmaceutical Nanotechnology, Department of Pharmaceutics, National Institute of Pharmaceutical Education and Research (NIPER), S.A.S. Nagar, Sector 67, Mohali, Punjab 160062, India.
Centre for Pharmaceutical Nanotechnology, Department of Pharmaceutics, National Institute of Pharmaceutical Education and Research (NIPER), S.A.S. Nagar, Sector 67, Mohali, Punjab 160062, India.
出版信息
Biomater Adv. 2024 Jan;156:213700. doi: 10.1016/j.bioadv.2023.213700. Epub 2023 Nov 14.
In this study, we investigated the potential of the sorafenib (SOR) and simvastatin (SIM) combination to induce ferroptosis-mediated cancer therapy. To enhance targeted drug delivery, we encapsulated the SOR + SIM combination within 4-carboxy phenylboronic acid (CPBA) modified PLGA nanoparticles (CPBA-PLGA(SOR + SIM)-NPs). The developed CPBA-PLGA(SOR + SIM)-NPs exhibited a spherical shape with a size of 213.1 ± 10.9 nm, a PDI of 0.22 ± 0.03, and a Z-potential of -22.9 ± 3.2 mV. Notably, these nanoparticles displayed faster drug release at acidic pH compared to physiological pH. In cellular experiments, CPBA-PLGA(SOR + SIM)-NPs demonstrated remarkable improvements, leading to a 2.51, 2.69, and 2.61-fold decrease in IC compared to SOR alone, and a 7.50, 16.71, and 5.11-fold decrease in IC compared to SIM alone in MDA-MB-231, A549, and HeLa cells, respectively. Furthermore, CPBA-PLGA(SOR + SIM)-NPs triggered a reduction in glutathione (GSH) levels, an increase in malondialdehyde (MDA) levels, and mitochondrial membrane depolarization in all three cell lines. Pharmacokinetic evaluation revealed a 2.50- and 2.63-fold increase in AUC, as well as a 1.53- and 2.46-fold increase in mean residence time (MRT) for SOR and SIM, respectively, compared to the free drug groups. Notably, the CPBA-PLGA(SOR + SIM)-NPs group exhibited significant reduction in tumor volume, approximately 9.17, 2.45, and 1.63-fold lower than the control, SOR + SIM, and PLGA(SOR + SIM)-NPs groups, respectively. Histological examination and biomarker analysis showed no significant differences compared to the control group, suggesting the biocompatibility of the developed particles for in-vivo applications. Altogether, our findings demonstrate that CPBA-PLGA(SOR + SIM)-NPs hold tremendous potential as an efficient drug delivery system for inducing ferroptosis, providing a promising therapeutic option for cancer treatment.
在这项研究中,我们研究了索拉非尼(SOR)和辛伐他汀(SIM)联合诱导铁死亡介导的癌症治疗的潜力。为了增强靶向药物递送,我们将 SOR+SIM 联合包封在 4-羧基苯硼酸(CPBA)修饰的 PLGA 纳米粒子(CPBA-PLGA(SOR+SIM)-NPs)中。所开发的 CPBA-PLGA(SOR+SIM)-NPs 呈球形,粒径为 213.1±10.9nm,PDI 为 0.22±0.03,Zeta 电位为-22.9±3.2mV。值得注意的是,与生理 pH 值相比,这些纳米粒子在酸性 pH 值下表现出更快的药物释放。在细胞实验中,CPBA-PLGA(SOR+SIM)-NPs 表现出显著的改善,导致 MDA-MB-231、A549 和 HeLa 细胞中 SOR 单独的 IC 降低了 2.51、2.69 和 2.61 倍,SIM 单独的 IC 降低了 7.50、16.71 和 5.11 倍。此外,CPBA-PLGA(SOR+SIM)-NPs 导致三种细胞系中的谷胱甘肽(GSH)水平降低,丙二醛(MDA)水平升高和线粒体膜去极化。药代动力学评价显示,与游离药物组相比,SOR 和 SIM 的 AUC 分别增加了 2.50 倍和 2.63 倍,平均驻留时间(MRT)分别增加了 1.53 倍和 2.46 倍。值得注意的是,CPBA-PLGA(SOR+SIM)-NPs 组的肿瘤体积显著减小,分别比对照组、SOR+SIM 组和 PLGA(SOR+SIM)-NPs 组低约 9.17、2.45 和 1.63 倍。组织学检查和生物标志物分析与对照组相比无显著差异,表明所开发的颗粒具有用于体内应用的生物相容性。总的来说,我们的研究结果表明,CPBA-PLGA(SOR+SIM)-NPs 作为一种有效的铁死亡诱导药物递送系统具有巨大的潜力,为癌症治疗提供了一种有前途的治疗选择。
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