College of Pharmacy, Keimyung University, Daegu, 42602, Republic of Korea; Department of Precision Medicine, School of Medicine, Sungkyunkwan University, Suwon, Gyeonggi, 16419, Republic of Korea.
Department of Immunology, School of medicine, Keimyung University, Daegu, Republic of Korea.
Biomaterials. 2025 Jan;312:122733. doi: 10.1016/j.biomaterials.2024.122733. Epub 2024 Jul 30.
Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) demonstrates unique characteristics in anticancer therapies as it selectively induces apoptosis in cancer cells. However, most cancer cells are TRAIL-resistant. Odanacatib (ODN), a cathepsin K inhibitor, is considered a novel sensitizer for cancer treatment. Combination therapy between TRAIL and sensitizers is considered a potent platform that improves TRAIL-based anticancer therapies beyond TRAIL monotherapy. Herein, we developed ODN loaded poly(lactic-co-glycolic) nanoparticles conjugated to GST-TRAIL (TRAIL-ODN-PLGA-NPs) to target and treat TRAIL-resistant cancer. TRAIL-ODN-PLGA-NPs demonstrated a significant increase in cellular uptake via death receptors (DR5 and DR4) on surface of cancer cells. TRAIL-ODN-PLGA-NPs exposure destroyed more TRAIL-resistant cells compared to a single treatment with free drugs. The released ODN decreased the Raptor protein, thereby increasing damage to mitochondria by elevating reactive oxygen species (ROS) generation. Additionally, Bim protein stabilization improved TRAIL-resistant cell sensitization to TRAIL-induced apoptosis. The in vivo biodistribution study revealed that TRAIL-ODN-PLGA-NPs demonstrated high location and retention in tumor sites via the intravenous route. Furthermore, TRAIL-ODN-PLGA-NPs significantly inhibited xenograft tumor models of TRAIL-resistant Caki-1 and TRAIL-sensitive MDA-MB-231 cells.The inhibition was associated with apoptosis activation, Raptor protein stabilizing Bim protein downregulation, Bax accumulation, and mitochondrial ROS generation elevation. Additionally, TRAIL-ODN-PLGA-NPs affected the tumor microenvironment by increasing tumor necrosis factor-α and reducing interleukin-6. In conclusion, we evealed that our formulation demonstrated synergistic effects against TRAIL compared with the combination of free drug in vitro and in vivo models. Therefore, TRAIL-ODN-PLGA-NPs may be a novel candidate for TRAIL-induced apoptosis in cancer treatment.
肿瘤坏死因子相关凋亡诱导配体(TRAIL)在癌症治疗中具有独特的特性,因为它选择性地诱导癌细胞凋亡。然而,大多数癌细胞对 TRAIL 具有抗性。odanacatib(ODN),一种组织蛋白酶 K 抑制剂,被认为是一种新的癌症治疗增敏剂。TRAIL 与增敏剂的联合治疗被认为是一种强大的平台,可以提高基于 TRAIL 的癌症治疗效果,超过 TRAIL 单药治疗。在此,我们开发了 GST-TRAIL 偶联的 ODN 负载的聚(乳酸-共-乙醇酸)纳米粒子(TRAIL-ODN-PLGA-NPs),以靶向和治疗 TRAIL 耐药的癌症。TRAIL-ODN-PLGA-NPs 通过癌细胞表面的死亡受体(DR5 和 DR4)显著增加了细胞摄取。与游离药物单一治疗相比,TRAIL-ODN-PLGA-NPs 暴露破坏了更多的 TRAIL 耐药细胞。释放的 ODN 降低了 Raptor 蛋白,从而通过增加活性氧(ROS)的产生来增加线粒体的损伤。此外,Bim 蛋白的稳定增加了 TRAIL 耐药细胞对 TRAIL 诱导的凋亡的敏感性。体内生物分布研究表明,TRAIL-ODN-PLGA-NPs 通过静脉途径在肿瘤部位具有高定位和保留。此外,TRAIL-ODN-PLGA-NPs 显著抑制了 TRAIL 耐药的 Caki-1 和 TRAIL 敏感的 MDA-MB-231 细胞的异种移植肿瘤模型。抑制与凋亡激活、Raptor 蛋白稳定 Bim 蛋白下调、Bax 积累和线粒体 ROS 生成增加有关。此外,TRAIL-ODN-PLGA-NPs 通过增加肿瘤坏死因子-α和降低白细胞介素-6 来影响肿瘤微环境。总之,我们揭示了我们的制剂在体外和体内模型中与游离药物联合使用相比,对 TRAIL 表现出协同作用。因此,TRAIL-ODN-PLGA-NPs 可能是癌症治疗中 TRAIL 诱导凋亡的一种新的候选药物。
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