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A convex optimization approach to cancer treatment to address tumor heterogeneity and imperfect drug penetration in physiological compartments

机译:一种凸面优化的癌症治疗方法,可解决肿瘤异质性和不完美的药物在生理区室中渗透的问题

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The clinical success of targeted cancer therapies is limited by the emergence of drug resistance often due to pre-existing tumor genetic heterogeneity and acquired, therapy-induced resistance. Targeted therapies have varied success in addressing metastatic disease, due to their ability to penetrate certain physiological compartments. This paper considers an evolutionary cancer model that incorporates tumor cell growth, mutation and compartmental migration and leverages recent results on the optimal control of monotone and convex systems to synthesize switching treatment strategies where a single drug or a predetermined combination of drugs is used at a given time. The need for switching is motivated by clinical considerations such as the limited effectiveness of any single targeted therapy against multiple resistance mechanisms arising in a single patient and the inability to design drug combinations at effective doses due to toxicity constraints. An optimal and clinically feasible switching therapy is obtained as the solution of a convex optimization problem that exploits the diagonally-dominant structure of the model. We demonstrate that this method yields an effective strategy in mitigating disease evolution in the presence of imperfect drug penetration in two compartments on an experimentally identified model of anaplastic lymphoma kinase (ALK)-rearranged lung carcinoma.
机译:靶向抗癌治疗的临床成功受到耐药性的出现的限制,这种耐药性的出现通常归因于预先存在的肿瘤遗传异质性以及获得性,治疗性诱导的耐药性。靶向疗法由于能够穿透某些生理区室而在解决转移性疾病方面取得了各种成功。本文考虑了一种融合了肿瘤细胞生长,突变和区室迁移的进化癌症模型,并利用了最近对单调和凸系统的最佳控制的结果来综合了在给定的情况下使用单一药物或预定药物组合的转换治疗策略。时间。出于临床考虑,例如针对单个患者中出现的针对多种耐药机制的任何单一靶向疗法的疗效有限,以及由于毒性限制而无法设计有效剂量的药物组合,促使人们需要进行转换。获得了最佳且临床上可行的转换疗法,作为利用模型对角线主导结构的凸优化问题的解决方案。我们证明,该方法产生了一种有效的策略,可以在不完整的药物渗透在两个间室上对变性变性淋巴瘤激酶(ALK)重新排列的肺癌进行实验鉴定的模型中,减轻疾病的发展。

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