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首页> 外文期刊>International Journal of Nanomedicine >In vitro Ultrasonic Potentiation of 2-Phenylethynesulfonamide/Magnetic Fluid Hyperthermia Combination Treatments for Ovarian Cancer
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In vitro Ultrasonic Potentiation of 2-Phenylethynesulfonamide/Magnetic Fluid Hyperthermia Combination Treatments for Ovarian Cancer

机译:2-苯基乙烯酰胺/磁性流体热疗组合治疗卵巢癌的体外超声升级

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Background: Magnetic Fluid Hyperthermia (MFH) is a promising adjuvant for chemotherapy, potentiating the action of anticancer agents. However, drug delivery to cancer cells must be optimized to improve the overall therapeutic effect of drug/MFH combination treatments. Purpose: The aim of this work was to demonstrate the potentiation of 2-phenylethynesulfonamide (PES) at various combination treatments with MFH, using low-intensity ultrasound as an intracellular delivery enhancer. Methods: The effect of ultrasound (US), MFH, and PES was first evaluated individually and then as combination treatments. Definitysup?/sup microbubbles and polyethylene glycol (PEG)-coated iron oxide nanoparticles were used to induce cell sonoporation and MFH, respectively. Assessment of cell membrane permeabilization was evaluated via fluorescence microscopy, iron uptake by cells was quantified by UV-Vis spectroscopy, and cell viability was determined using automatic cell counting. Results: Notable reductions in cancer cell viability were observed when ultrasound was incorporated. For example, the treatment US+PES reduced cell viability by 37% compared to the non-toxic effect of the drug. Similarly, the treatment US+MFH using mild hyperthermia (41°C), reduced cell viability by an additional 18% when compared to the effect of MH alone. Significant improvements were observed for the combination of US+PES+MFH with cell viability reduced by an additional 26% compared to the PES+MFH group. The improved cytotoxicity was attributed to enhanced drug/nanoparticle intracellular delivery, with iron uptake values nearly twice those achieved without ultrasound. Various treatment schedules were examined, and all of them showed substantial cell death, indicating that the time elapsed between sonoporation and magnetic field exposure was not significant. Conclusion: Superior cancer cell-killing patterns took place when ultrasound was incorporated thus demonstrating the in vitro ultrasonic potentiation of PES and mild MFH. This work demonstrated that ultrasound is a promising non-invasive enhancer of PES/MFH combination treatments, aiming to establish a sono-thermo-chemotherapy in the treatment of ovarian cancer.
机译:背景:磁性流体热疗(MFH)是一种有前途的化疗的佐剂,增强了抗癌剂的作用。然而,必须优化对癌细胞的药物递送,以改善药物/ MFH组合治疗的总体治疗效果。目的:本作作品的目的是在使用低强度超声作为细胞内递送增强剂的各种组合处理中证明2-苯基乙烯酰胺(PES)的增强。方法:首先单独评估超声(US),MFH和PE的效果,然后作为组合治疗评估。定义β微泡和聚乙二醇(PEG) - 涂层氧化铁纳米颗粒分别分别诱导细胞声孔和MFH。通过荧光显微镜评估细胞膜渗透性的评估,通过UV-Vis光谱量化细胞的铁吸收,使用自动细胞计数测定细胞活力。结果:当掺入超声时,观察到癌细胞活力的显着降低。例如,与药物的无毒作用相比,治疗US + PES减少了37%的细胞活力。类似地,使用轻度热疗(41℃)的治疗方法+ MFH,与单独的MH的效果相比,通过额外的18%降低细胞活力。与PES + MFH组相比,对US + PES + MFH的组合观察到US + PES + MFH的组合的显着改进。改进的细胞毒性归因于增强的药物/纳米粒子细胞内递送,铁吸收值几乎两倍于无超声波达到的。检查各种治疗时间表,所有这些治疗时间表都显示出大量的细胞死亡,表明声孔和磁场暴露之间经过的时间并不重要。结论:在掺入超声时发生了优异的癌细胞杀灭图案,从而证明了PE和轻度MFH的体外超声波升级。这项工作表明,超声波是PES / MFH组合治疗的有前途的非侵入性增强剂,旨在在卵巢癌治疗中建立一个Sono-Thermo-化疗。

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