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Optimal Scheduling of Therapy to Delay Cancer Drug Resistance

机译:延缓癌症耐药性的最佳调度

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One of the most difficult challenges in cancer therapy is the emergence of drug resistance within tumors. Sometimes drug resistance can emerge as the result of mutations and Darwinian selection. However, recently another phenomenon has been discovered, in which tumor cells switch back and forth between drug-sensitive and pre-resistant states. Upon exposure to the drug, sensitive cells die off, and pre-resistant cells become locked in to a state of permanent drug resistance. In this paper, we explore the implications of this transient state switching for therapy scheduling. We propose a model to describe the phenomenon and estimate parameters from experimental melanoma data. We then compare the performance of continuous and alternating drug schedules, and use sensitivity analysis to explore how different conditions affect the efficacy of each schedule. We find that for our estimated parameters, a continuous therapy schedule is optimal. However we also find that an alternating schedule can be optimal for other hypothetical parameter sets, depending on the difference in growth rate between pre-drug and post-drug cells, the delay between exposure to the drug and emergence of resistance, and the rates of switching between states.
机译:癌症治疗中最困难的挑战之一是肿瘤内耐药性的出现。由于突变和达尔文选择的结果,有时可以出现耐药性。然而,最近已经发现了另一种现象,其中肿瘤细胞在药物敏感和预抗性状态之间来回切换。在暴露于药物后,敏感细胞消耗,并且预抗性细胞被锁定到永久性耐药状态。在本文中,我们探讨了该瞬态状态切换进行治疗调度的影响。我们提出了一种模型来描述来自实验黑素瘤数据的现象和估算参数。然后,我们比较连续和交替的药物时间表的性能,并使用灵敏度分析来探讨不同的条件如何影响每个时分的功效。我们发现,对于我们的估计参数,连续治疗时间表是最佳的。然而,我们还发现交替的时间表可以对其他假设参数集最佳,这取决于预防药物和药物后细胞之间的生长速率差异,暴露于药物和抵抗的出现之间的延迟和抵抗力在状态之间切换。

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