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The multicellular tumor spheroid model for high-throughput cancer drug discovery

机译:用于高通量癌症药物发现的多细胞肿瘤球体模型

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For the past 30 years 2D-cell-based assay models have dominated preclinical cancer drug discovery efforts. 2D-cell-based models fail to predict in vivo efficacy, contributing to a lower success rate and higher cost required to translate an investigational new drug to clinical approval. Technological advances in 3D-cell culture models bridge the gap between 2D and in vivo models to improve upon the current success rates of cancer drug discovery. Areas covered: This review focuses on the multicellular tumor spheroid (MCTS), particularly how this model can be utilized for HTS drug discovery. We discuss the current technologies for uniform culture of MCTS suitable for HTS and detection methods utilized for assay development and drug screening. Expert opinion: Substantial hurdles remain before we reach the ultimate goal of robust HTS of large compound libraries with MCTS models. Specifically, we can group these challenges into three categories: MCTS growth, data collection, and data analysis. The MCTS model should be utilized with fluorescent readouts and high-content imaging with a systems biology approach to model human tumors in vitro. Such models will be more predictive of in vivo efficacy, improving on the current success rates of cancer drug discovery from bench to bedside.
机译:在过去的30年中,基于2D细胞的分析模型主导了临床前癌症药物发现工作。基于2D细胞的模型无法预测体内功效,导致将研究中的新药转化为临床批准品所需的成功率较低且成本较高。 3D细胞培养模型的技术进步弥合了2D模型与体内模型之间的鸿沟,以改善当前癌症药物发现的成功率。涵盖的领域:这篇综述着重于多细胞肿瘤球体(MCTS),特别是如何将该模型用于HTS药物发现。我们讨论了适用于HTS的MCTS统一培养的当前技术,以及用于分析开发和药物筛选的检测方法。专家意见:在达到使用MCTS模型建立大型化合物库的强大HTS的最终目标之前,还存在很多障碍。具体来说,我们可以将这些挑战分为三类:MCTS增长,数据收集和数据分析。 MCTS模型应与荧光读数和高内涵成像一起使用,并应采用系统生物学方法体外模拟人肿瘤。这样的模型将更好地预测体内功效,从而提高当前从实验台到床边发现癌症药物的成功率。

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