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Embedded multicellular spheroids as a biomimetic 3D cancer model for evaluating drug and drug-device combinations

机译:嵌入式多细胞球体作为仿生3D癌症模型,用于评估药物和药物设备组合

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摘要

Multicellular aggregates of cells, termed spheroids, are of interest for studying tumor behavior and for evaluating the response of pharmacologically active agents. Spheroids more faithfully reproduce the tumor macrostructure found invivo compared to classical 2D monolayers. We present a method for embedding spheroids within collagen gels followed by quantitative and qualitative whole spheroid and single cell analyses enabling characterization over the length scales from molecular to macroscopic. Spheroid producing and embedding capabilities are demonstrated for U2OS and MDA-MB-231 cell lines, of osteosarcoma and breast adenocarcinoma origin, respectively. Finally, using the MDA-MB-231 tumor model, the chemotherapeutic response between paclitaxel delivery as a bolus dose, as practiced in the clinic, is compared to delivery within an expansile nanoparticle. The expansile nanoparticle delivery route provides a superior outcome and the results mirror those observed in a murine xenograft model. These findings highlight the synergistic beneficial results that may arise from the use of a drug deliverysystem, and the need to evaluate both drug candidates and delivery systems in the research and preclinical screening phases of a new cancer therapy development program.
机译:细胞的多细胞聚集体,称为球状体,对于研究肿瘤行为和评估药理活性剂的反应非常重要。与经典2D单层相比,类球体更忠实地再现了体内发现的肿瘤宏观结构。我们提出了一种将球状体包埋在胶原蛋白凝胶中的方法,然后进行定量和定性的整个球状体和单细胞分析,从而能够表征从分子到宏观的长度范围。分别针对骨肉瘤和乳​​腺腺癌的U2OS和MDA-MB-231细胞系展示了球状体的产生和包埋能力。最后,使用MDA-MB-231肿瘤模型,将紫杉醇作为推注剂量的递送之间的化学治疗反应(如临床实践)与可膨胀纳米颗粒内的递送进行比较。膨胀的纳米颗粒递送途径提供了优异的结果,并且结果反映了在小鼠异种移植模型中观察到的结果。这些发现强调了使用药物输送系统可能产生的协同有益结果,以及在新的癌症治疗开发计划的研究和临床前筛查阶段需要评估候选药物和药物输送系统。

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