A novel combination therapy for ER+ breast cancer suppresses drug resistance via an evolutionary double-bind

Rena Emond, Jeffrey West, Vince Grolmusz, Patrick Cosgrove, Aritro Nath, Alexander R. A. Anderson, Andrea H. Bild
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Abstract

Chemotherapy remains a commonly used and important treatment option for metastatic breast cancer. A majority of ER+ metastatic breast cancer patients ultimately develop resistance to chemotherapy, resulting in disease progression. We hypothesized that an "evolutionary double-bind", where treatment with one drug improves the response to a different agent, would improve the effectiveness and durability of responses to chemotherapy. This approach exploits vulnerabilities in acquired resistance mechanisms. Evolutionary models can be used in refractory cancer to identify alternative treatment strategies that capitalize on acquired vulnerabilities and resistance traits for improved outcomes. To develop and test these models, ER+ breast cancer cell lineages sensitive and resistant to chemotherapy are grown in spheroids with varied initial population frequencies to measure cross-sensitivity and efficacy of chemotherapy and add-on treatments such as disulfiram combination treatment. Different treatment schedules then assessed the best strategy for reducing the selection of resistant populations. We developed and parameterized a game-theoretic mathematical model from this in vitro experimental data, and used it to predict the existence of a double-bind where selection for resistance to chemotherapy induces sensitivity to disulfiram. The model predicts a dose-dependent re-sensitization (a double-bind) to chemotherapy for monotherapy disulfiram.
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一种治疗ER+乳腺癌的新型联合疗法通过进化双结合抑制耐药性
化疗仍然是转移性乳腺癌常用的重要治疗方法。大多数ER+转移性乳腺癌患者最终会对化疗产生耐药性,导致疾病进展。我们假设 "进化双结合",即用一种药物治疗可改善对另一种药物的反应,从而提高化疗反应的有效性和持久性。这种方法利用了获得性抗药性机制的弱点。进化模型可用于难治性癌症,以确定替代治疗策略,利用获得性弱点和抗药性特征改善疗效。为了开发和测试这些模型,对化疗敏感和耐药的ER+乳腺癌细胞系被培养在具有不同初始群体频率的球体内,以测量化疗和附加治疗(如双硫嘧啶联合治疗)的交叉敏感性和疗效。然后根据不同的治疗方案评估减少耐药群体选择的最佳策略。我们根据这些体外实验数据建立了一个博弈论数学模型,并对其进行了参数化处理,用它来预测是否存在双重束缚,即对化疗的抗药性选择会诱发对双硫仑的敏感性。该模型预测了单药双硫仑对化疗的再敏感性(双结合)与剂量的关系。
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