Population pharmacokinetics modelling for clinical dose adjustment of carboplatin in dogs.

IF 2.3 2区 农林科学 Q1 VETERINARY SCIENCES BMC Veterinary Research Pub Date : 2024-12-23 DOI:10.1186/s12917-024-04404-1
Jérémy Béguin, Sarra Mahfoudhi, Marie Uzel, Antoine Rostang, Catherine Ibish, Aude A Ferran, Ludovic Pelligand, Anne Hulin, Matthias Kohlhauer
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Abstract

Background: Carboplatin is a human chemotherapeutic agent which is frequently used in dogs for the management of solid tumors. In human patient, its dosage is adjusted carefully, based on the creatinine clearance computation. In dogs however, the pharmacokinetics of carboplatin is poorly known and the dose 300 mg/m2 is based mostly on empirical data. Here, we aimed at characterizing the pharmacokinetics of carboplatin and determined the influence of several covariates, including creatinine plasma concentration and neutering status, in dogs, and used this model to predict myelotoxicity.

Results: Sixteen client owned dogs were included after carboplatin administration (300 mg/m2). For each animals, three to four plasma samples were collected and free plasma concentration of carboplatin was determined by HPLC/MS and analysed using Monolix® software with Non-linear mixed effect modelling. A mono-compartmental model best described the plasma concentration of carboplatin with log plasma creatinine concentration and sterilization status as covariates. After adjustment with the covariates, median population clearance was 3.62 [3.15 - 4.12] L/h/kg and volume of distribution was 3.93 [3.84 - 4.14] L/kg. The application of this model in 14 additional dogs demonstrates that individual drug exposure (model-predicted Area Under the Curve) predicted thrombocyte blood reduction (Pearson coefficient r2 = 0.73, p = 0.002) better than dose after 14 days following administration of carboplatin.

Conclusion: Based on our results, plasma creatinine concentration and the sterilization status are relevant explanatory covariates for the pharmacokinetics variability of carboplatin in client owned dogs. Dose adjustment based on these parameters could represent a promising strategy for minimizing thrombocyte toxicity.

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犬卡铂临床剂量调整的群体药代动力学模型。
背景:卡铂是一种人类化疗药物,经常用于狗的实体肿瘤治疗。在人类患者中,它的剂量是根据肌酐清除率的计算来仔细调整的。然而,在狗身上,卡铂的药代动力学知之甚少,300mg /m2的剂量主要基于经验数据。在这里,我们的目的是表征卡铂的药代动力学,并确定几个协变量的影响,包括肌酸酐血浆浓度和狗的绝育状态,并使用该模型预测骨髓毒性。结果:16只患者自养犬在卡铂(300 mg/m2)治疗后纳入研究。每只动物采集3 - 4个血浆样本,用HPLC/MS测定游离血浆卡铂浓度,并使用Monolix®软件进行非线性混合效应建模分析。单室模型以对数血浆肌酐浓度和灭菌状态作为协变量,最好地描述了卡铂的血浆浓度。经协变量调整后,中位人群清除率为3.62 [3.15 - 4.12]L/h/kg,分布容积为3.93 [3.84 - 4.14]L/kg。该模型在另外14只狗身上的应用表明,个体药物暴露(模型预测的曲线下面积)预测血小板血减少(Pearson系数r2 = 0.73, p = 0.002)优于卡铂给药后14天的剂量。结论:根据我们的研究结果,血浆肌酐浓度和灭菌状态是卡铂在客户养狗体内药代动力学变异性的相关解释协变量。基于这些参数的剂量调整可能是最小化血小板毒性的一种有希望的策略。
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来源期刊
BMC Veterinary Research
BMC Veterinary Research VETERINARY SCIENCES-
CiteScore
4.80
自引率
3.80%
发文量
420
审稿时长
3-6 weeks
期刊介绍: BMC Veterinary Research is an open access, peer-reviewed journal that considers articles on all aspects of veterinary science and medicine, including the epidemiology, diagnosis, prevention and treatment of medical conditions of domestic, companion, farm and wild animals, as well as the biomedical processes that underlie their health.
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