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Second-order effects of chemotherapy pharmacodynamics and pharmacokinetics on tumor regression and cachexia

Second-order effects of chemotherapy pharmacodynamics and pharmacokinetics on tumor regression and cachexia

来源:bioRxiv_logobioRxiv
英文摘要

Drug dose response curves are ubiquitous in cancer biology, but these curves are often used to mea- sure differential response in first-order effects: the effectiveness of increasing the cumulative dose delivered. In contrast, second-order effects (the variance of drug dose) are often ignored. Knowledge of second-order effects may improve the design of chemotherapy scheduling protocols, leading to improvements in tumor response without changing the total dose delivered. By considering treatment schedules with identical cumulative dose delivered, we optimize treatment by comparing high variance schedules (e.g. high dose, low dose) with low variance schedules (constant dose). We extend a previous framework used to quantify second-order effects, known as antifragility theory, to investigate the role of drug pharmacokinetics. Using a simple one-compartment model, we find that high variance schedules are effective for a wide range of cumulative dose values. Next, using a mouse-parameterized two-compartment model of 5-fluorouracil, we show that the optimal schedule depends on initial tumor volume. Finally, we illustrate the trade-off between tumor response and lean mass preservation. Mathematical modeling indicates that high variance dose schedules provide a potential path forward in mitigating the risk of chemotherapy-associated cachexia by preserving lean mass without sacrificing tumor response.

Pierik Luke、Anderson Alexander R. A.、McDonald Patricia、West Jeffrey

10.1101/2023.06.14.544974

医药卫生理论医学研究方法肿瘤学

Pierik Luke,Anderson Alexander R. A.,McDonald Patricia,West Jeffrey.Second-order effects of chemotherapy pharmacodynamics and pharmacokinetics on tumor regression and cachexia[EB/OL].(2025-03-28)[2025-05-16].https://www.biorxiv.org/content/10.1101/2023.06.14.544974.点此复制

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