伴随用药与循环肿瘤细胞:是友是敌?

IF 4.6 Q1 ONCOLOGY 癌症耐药(英文) Pub Date : 2023-01-01 DOI:10.20517/cdr.2022.68
Serena Di Cosimo, Vera Cappelletti
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引用次数: 0

摘要

几乎在全球范围内都观察到癌症患者同时使用药物;然而,在医学文献中很少关注这一主题。大多数临床研究没有描述纳入时和治疗期间使用的药物的类型和持续时间,也没有描述这些药物如何影响实验和/或标准治疗。关于伴随药物与肿瘤生物标志物之间潜在相互作用的信息甚至更少。然而,我们确实知道,伴随药物会使癌症临床试验和生物标志物的开发复杂化,从而导致它们之间的相互作用,导致副作用,并导致抗癌治疗的依从性不理想。基于这些前提,并从Jurisova等人的研究出发,该研究报道了常用药物对乳腺癌女性预后的影响以及循环肿瘤细胞(CTCs)的检测,我们评论了CTCs作为一种新兴的乳腺癌诊断和预后工具的作用。我们还报道了CTC与其他肿瘤和血液成分相互作用的已知和假设机制,可能受到广泛的药物(包括非处方药)的调节,并讨论了常用的伴随药物对CTC检测和清除的可能影响。综上所述,可以想象,伴随药物不一定是一个问题,相反,它们的良性机制可以被利用来减少肿瘤的扩散,增强抗癌治疗的效果。
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Concomitant medications and circulating tumor cells: friends or foes?

The use of concomitant medications by patients with cancer is observed almost globally; however, little attention has been paid to this topic in the medical literature. Most clinical studies do not describe the type and duration of drugs used at the time of inclusion and during treatment or how these drugs may affect the experimental and/or standard therapy. Even less information has been published on the potential interaction between concomitant medications and tumor biomarkers. However, we do know that concomitant drugs can complicate cancer clinical trials and biomarker development, thus contributing to their interaction, leading to side effects, and resulting in suboptimal adherence to anticancer treatment. On the basis of these premises and moving from the study by Jurisova et al., which reported the effect of commonly used drugs on the prognosis of women with breast cancer and the detection of circulating tumor cells (CTCs), we comment on the role of CTCs as an emerging diagnostic and prognostic tool for breast cancer. We also report the known and hypothesized mechanisms of CTC interplay with other tumor and blood components, possibly modulated by widespread drugs, including over-the-counter compounds, and discuss the possible implications of commonly used concomitant medications on CTC detection and clearance. After considering all these points, it is conceivable that concomitant drugs are not necessarily a problem, but on the contrary, their virtuous mechanisms can be exploited to reduce tumor spread and enhance the effect of anticancer therapies.

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