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3D Cultures of Prostate Cancer Cells Cultured in a Novel High-Throughput Culture Platform Are More Resistant to Chemotherapeutics Compared to Cells Cultured in Monolayer

机译:与单层培养的细胞相比在新型高通量培养平台上培养的前列腺癌细胞的3D培养对化学疗法的抵抗力更高

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摘要

Despite monolayer cultures being widely used for cancer drug development and testing, 2D cultures tend to be hypersensitive to chemotherapy and are relatively poor predictors of whether a drug will provide clinical benefit. Whilst generally more complicated, three dimensional (3D) culture systems often better recapitulate true cancer architecture and provide a more accurate drug response. As a step towards making 3D cancer cultures more accessible, we have developed a microwell platform and surface modification protocol to enable high throughput manufacture of 3D cancer aggregates. Herein we use this novel system to characterize prostate cancer cell microaggregates, including growth kinetics and drug sensitivity. Our results indicate that prostate cancer cells are viable in this system, however some non-cancerous prostate cell lines are not. This system allows us to consistently control for the presence or absence of an apoptotic core in the 3D cancer microaggregates. Similar to tumor tissues, the 3D microaggregates display poor polarity. Critically the response of 3D microaggregates to the chemotherapeutic drug, docetaxel, is more consistent with in vivo results than the equivalent 2D controls. Cumulatively, our results demonstrate that these prostate cancer microaggregates better recapitulate the morphology of prostate tumors compared to 2D and can be used for high-throughput drug testing.
机译:尽管单层培养物已广泛用于癌症药物的开发和测试,但二维培养物对化学疗法还是非常敏感的,并且对于药物是否会提供临床益处的预测相对较差。尽管通常更为复杂,但三维(3D)培养系统通常可以更好地概括真实的癌症结构,并提供更准确的药物反应。为了使3D癌症文化更容易获得,我们开发了微孔平台和表面修饰方案,可实现3D癌症聚集体的高通量生产。本文中,我们使用这个新颖的系统来表征前列腺癌细胞微聚集体,包括生长动力学和药物敏感性。我们的结果表明,前列腺癌细胞在该系统中是可行的,但是某些非癌性前列腺细胞系却不可行。该系统使我们能够一致地控制3D癌症微聚集体中是否存在凋亡核心。与肿瘤组织相似,3D微聚集体显示出不良的极性。至关重要的是,与等效的2D对照相比,3D微聚集体对化学治疗药物多西紫杉醇的反应与体内结果更加一致。累积地,我们的结果表明,与2D相比,这些前列腺癌微聚集体更好地概括了前列腺肿瘤的形态,可用于高通量药物测试。

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