A Prospective Pharmacokinetic Study of Docetaxel in Breast Cancer Patients in Relation to CYP3A4 Activity

Mervat Mostafa Omran, O. Badary, A. Helal, S. Shouman
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引用次数: 5

Abstract

Abstract Purpose: To study the correlation between pharmacokinetics & pharmacodynamic of docetaxel and CYP3A4 activity in Egyptian cancer patients. Patients and methods: Fourteen Egyptian female Patients with metastatic breast cancer, World Health Organization (WHO) performance status 0 to 2, had received prior chemotherapy regimen, were treated with single-agent docetaxel (100 mg/m2), given every 21 days. Hydrocortisone 300 mg IV was administered 2 days before docetaxel treatment and Cytochrome 3A4 activity was determined by measuring the level of urinary metabolites of 6β-hydroxy cortisol (6β-OHF) and cortisol (FC). For the pharmacokinetic study, Blood samples were taken before and after IV infusion for 1 hr of 100 mg/m2 docetaxel. The level of the drug was determined using HPLC and the correlation between pharmacokinetics and CYP3A4 activity were determined. Results: After cortisol administration, the total amount of 24-hour urinary 6β-OHF and FC were19.97 ± 10.43 and 16.84 ± 10.36 mg/24 h (mean ± SD) respectively. On the other hand, the 6β-OHF/FC ratio after cortisol administration was 1.86 ± 1.933. The pharmacokinetic parameters of docetaxel were clearance 19.9 ± 4.5 L/hr, the volume of distribution 65.6 ± 28.6 L (mean ± SD) and AUC 7.2 μg/ml.hr (range 5-8.8 μg/ml.hr) ± SD). A significant correlation was found between 6β-OHF/FC ratio and neutropenia (p=0.04) in addition correlation between 6β-OHF and Cmax (p=0.04). Conclusion: The interpatient variability of CYP3A4 activity in each patient could be predicted by measuring the total amount of 24 hour urinary 63-OHF after cortisol administration. Individualized dosing to optimize drug exposure for each patient could be performed based on this method. A farther study of fixed versus individualized dosing of docetaxel is needed to determine whether individualized chemotherapy with the application of this method can reduce PK and toxicity variability.
多西紫杉醇对乳腺癌患者CYP3A4活性影响的前瞻性药代动力学研究
摘要目的:研究多西他赛药动学和药效学与埃及肿瘤患者CYP3A4活性的相关性。患者和方法:14例埃及女性转移性乳腺癌患者,世界卫生组织(WHO)评分为0 ~ 2,既往接受化疗方案,多西他赛单药治疗(100 mg/m2),每21天给药一次。在多西他赛治疗前2天给予氢化可的松300 mg IV,通过测定尿中6β-羟基皮质醇(6β-OHF)和皮质醇(FC)的代谢物水平来测定细胞色素3A4的活性。为了进行药代动力学研究,在静脉输注100 mg/m2多西紫杉醇1小时前后取血样。采用高效液相色谱法测定药物水平,并测定药代动力学与CYP3A4活性的相关性。结果:皮质醇给药后,24小时尿6β-OHF和FC总量分别为19.97±10.43和16.84±10.36 mg/24 h (mean±SD)。另一方面,皮质醇处理后6β-OHF/FC比值为1.86±1.933。多西他赛的清除率为19.9±4.5 L/hr,分布容积为65.6±28.6 L (mean±SD), AUC为7.2 μg/ml。(范围5-8.8 μg/ml.hr)±SD)。6β-OHF/FC与中性粒细胞减少症有显著相关(p=0.04), 6β-OHF与Cmax有显著相关(p=0.04)。结论:通过测量皮质醇给药后24小时尿63-OHF总量,可以预测患者间CYP3A4活性的变异性。个体化给药以优化每位患者的药物暴露,可基于该方法进行。需要进一步研究多西他赛的固定剂量和个体化剂量,以确定应用该方法进行个体化化疗是否可以降低PK和毒性变异性。
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