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A Strategy to Delay the Development of Cisplatin Resistance by Maintaining a Certain Amount of Cisplatin-Sensitive Cells

机译:通过维持一定量的顺铂敏感细胞来延迟顺铂耐药性发展的策略

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摘要

Cisplatin (ddp), which is commonly employed in the treatment of many advanced cancers, often results in initial therapeutic success; however, rapid progression of ddp-resistant cells remains the main reason for treatment failure. Facd with such a problem, we investigated the fitness differences between ddp-sensitive and ddp-resistant cell lines. We found that the growth of ddp-resistant cells was significantly slower than that of sensitive cells due to elevated ROS levels, which suggested that the ddp resistance mechanisms may have negative impacts on the growth of resistant cells. Furthermore, we observed that, when mixed with ddp-sensitive cells, ddp-resistant cells failed to compete, and the growth of ddp-resistant cells could therefore be suppressed by treatment in vivo. We propose a mathematical model parameterized based on in vivo experiments to describe the allometric growth of tumors consisting of two competing subclones. According to our model, a quantitative strategy with a variant drug-dosing interval is proposed to control tumor growth. Taking advantage of intratumoral competition, our strategy with appropriate dosing intervals could remarkably delay the development of ddp resistance and prolong overall survival. Maintaining a certain number of ddp-sensitive cells rather than eradicating the tumor with continuous treatment is feasible for future tumor treatment.
机译:顺铂(ddp)通常用于治疗许多晚期癌症,通常会产生初步的治疗成功;然而,ddp耐药细胞的快速发展仍然是治疗失败的主要原因。面对这样的问题,我们研究了ddp敏感和ddp耐药细胞系之间的适应性差异。我们发现由于ROS水平升高,ddp耐药细胞的生长明显慢于敏感细胞,这表明ddp耐药机制可能对耐药细胞的生长产生负面影响。此外,我们观察到,当与ddp敏感细胞混合时,ddp耐药细胞无法竞争,因此可以通过体内治疗抑制ddp耐药细胞的生长。我们提出了基于体内实验参数化的数学模型,以描述由两个竞争亚克隆组成的肿瘤的异形生长。根据我们的模型,提出了一种具有可变给药间隔的定量策略,以控制肿瘤的生长。利用肿瘤内竞争的优势,我们的策略以适当的给药间隔可以显着延迟ddp耐药性的发展并延长总体生存期。维持一定数量的ddp敏感细胞而不是通过连续治疗根除肿瘤对于将来的肿瘤治疗是可行的。

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