首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Coadministration of a tumor-penetrating peptide improves the therapeutic efficacy of paclitaxel in a novel air-grown lung cancer 3D spheroid model
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Coadministration of a tumor-penetrating peptide improves the therapeutic efficacy of paclitaxel in a novel air-grown lung cancer 3D spheroid model

机译:肿瘤渗透肽的共同分析可提高紫杉醇在新型空气生长的肺癌3D球状体模型中的治疗效果

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摘要

Three-dimensional (3 D) cell culture platforms are increasingly being used in cancer research and drug development since they mimic avascular tumors in vitro. In this study, we focused on the development of a novel air-grown multicellular spheroid (MCS) model to mimic in vivo tumors for understanding lung cancer biology and improvement in the evaluation of aerosol anticancer therapeutics. 3 D MCS were formed using A549 lung adenocarcinoma cells, comprising cellular heterogeneity with respect to different proliferative and metabolic gradients. The growth kinetics, morphology and 3 D structure of air-grown MCS were characterized by brightfield, fluorescent and scanning electron microscopy. MCS demonstrated a significant decrease in growth when the tumor-penetrating peptide iRGD and paclitaxel (PTX) were coadministered as compared with PTX alone. It was also found that when treated with both iRGD and PTX, A549 MCS exhibited an increase in apoptosis and decrease in clonogenic survival capacity in contrast to PTX treatment alone. This study demonstrated that coadministration of iRGD resulted in the improvement of the tumor penetration ability of PTX in an in vitro A549 3 D MCS model. In addition, this is the first time a high-throughput air-grown lung cancer tumor spheroid model has been developed and evaluated.
机译:三维(3D)细胞培养平台越来越多地用于癌症研究和药物开发,因为它们在体外模仿缺血肿瘤。在这项研究中,我们专注于开发一种新型空气种植的多细胞球体(MCS)模型,以模仿体内肿瘤,以了解肺癌生物学和改善气溶胶抗癌治疗剂评价。使用A549肺腺癌细胞形成3D MCS,其包含相对于不同增殖和代谢梯度的细胞异质性。通过波纹,荧光和扫描电子显微镜表征空气生长MCS的生长动力学,形态和3d结构。当与单独的PTX相比,MCS当肿瘤穿透肽IRGD和PACLITAXEL(PTX)相比,MCS显着降低。还发现,当用IRGD和PTX治疗时,A549 MCS呈上凋亡的增加,并与单独的PTX治疗相比,克隆源性存活能力降低。该研究表明IRGD的共同分子导致PTX在体外A549 3 D MCS模型中的肿瘤渗透能力提高。此外,这是第一次开发和评估了高通量空气生长的肺癌肿瘤球状体型。

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