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Dynamic Rearrangement of Cell States Detected by Systematic Screening of Sequential Anticancer Treatments

机译:系统筛选序贯抗癌治疗检测细胞状态的动态重排

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摘要

Signaling networks are nonlinear and complex, involving a large ensemble of dynamic interaction states that fluctuate in space and time. However, therapeutic strategies, such as combination chemotherapy, rarely consider the timing of drug perturbations. If we are to advance drug discovery for complex diseases, it will be essential to develop methods capable of identifying dynamic cellular responses to clinically relevant perturbations. Here, we present a Bayesian dose-response framework and the screening of an oncological drug matrix, comprising 10,000 drug combinations in melanoma and pancreatic cancer cell lines, from which we predict sequentially effective drug combinations. Approximately 23% of the tested combinations showed high-confidence sequential effects (either synergistic or antagonistic), demonstrating that cellular perturbations of many drug combinations have temporal aspects, which are currently both underutilized and poorly understood.
机译:信号网络是非线性的且复杂的,涉及大量随时间和空间波动的动态交互状态。但是,诸如联合化疗等治疗策略很少考虑药物扰动的时机。如果我们要促进复杂疾病的药物发现,那么开发能够识别对临床相关扰动的动态细胞反应的方法将至关重要。在这里,我们介绍了贝叶斯剂量反应框架和肿瘤药物基质的筛选,包括黑色素瘤和胰腺癌细胞系中的10,000种药物组合,从中我们可以依次预测有效的药物组合。大约23%的测试组合显示出高置信度的顺序效应(协同或拮抗),表明许多药物组合的细胞扰动具有暂时性,目前尚未得到充分利用和了解。

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