Cancer Research Center of Toulouse (CRCT), Inserm U1037, Université Paul Sabatier - Toulouse III, 2 Avenue Hubert Curien, Toulouse 31100, France.
Institut Claudius Regaud, Institut Universitaire du Cancer de Toulouse - Oncopole, Toulouse, France.
Eur J Pharm Sci. 2024 Aug 1;199:106809. doi: 10.1016/j.ejps.2024.106809. Epub 2024 May 22.
Letrozole, an aromatase inhibitor metabolised via CYP2A6 and CYP3A4/5 enzymes, is used as adjuvant therapy for women with hormone receptor (HR)-positive early breast cancer. The objective of this study was to quantify the impact of CYP2A6 genotype on letrozole pharmacokinetics (PK), to identify non-adherent patients using a population approach and explore the possibility of a relationship between non-adherence and early relapse.
Breast cancer patients enrolled in the prospective PHACS study (ClinicalTrials.gov NCT01127295) and treated with adjuvant letrozole 2.5 mg/day were included. Trough letrozole concentrations (C) were measured every 6 months for 3 years by a validated LC-MS/MS method. Concentration-time data were analysed using non-linear mixed effects modelling. Three methods were evaluated for identification of non-adherent subjects using the base PK model.
617 patients contributing 2534 plasma concentrations were included and led to a one-compartment PK model with linear absorption and elimination. Model-based methods identified 28 % of patients as non-adherent based on high fluctuations of their C compared to 3 % based on patient declarations. The covariate analysis performed in adherent subjects revealed that CYP2A6 intermediate (IM) and slow metabolisers (SM) had 21 % (CI95 % = 12 - 30 %) and 46 % (CI95 % = 41 - 51 %) lower apparent clearance, respectively, compared to normal and ultrarapid metabolisers (NM+UM). Early relapse (19 patients) was not associated with model-estimated, concentration-based or declared adherence in the total population (p = 0.41, p = 0.37 and p = 0.45, respectively).
These findings will help future investigations focusing on the exposure-efficacy relationship for letrozole in adjuvant setting.
来曲唑是一种通过 CYP2A6 和 CYP3A4/5 酶代谢的芳香酶抑制剂,用于治疗激素受体(HR)阳性早期乳腺癌的辅助治疗。本研究的目的是量化 CYP2A6 基因型对来曲唑药代动力学(PK)的影响,使用群体方法识别不依从的患者,并探索不依从与早期复发之间的关系。
纳入前瞻性 PHACS 研究(ClinicalTrials.gov NCT01127295)并接受辅助来曲唑 2.5mg/天治疗的乳腺癌患者。通过验证的 LC-MS/MS 方法每 6 个月测量 3 年的来曲唑谷浓度(C)。使用非线性混合效应模型分析浓度-时间数据。使用基础 PK 模型评估了三种方法来识别不依从的受试者。
617 名患者共贡献 2534 个血浆浓度,导致单室 PK 模型,具有线性吸收和消除。基于模型的方法根据 C 的高波动将 28%的患者识别为不依从,而基于患者声明的方法仅识别 3%的患者为不依从。在依从性受试者的协变量分析中,发现 CYP2A6 中间代谢型(IM)和慢代谢型(SM)的表观清除率分别比正常和超快代谢型(NM+UM)低 21%(95%CI95%=12-30%)和 46%(95%CI95%=41-51%)。在总人群中,早期复发(19 名患者)与模型估计的、基于浓度的或声明的依从性无关(p=0.41,p=0.37 和 p=0.45,分别)。
这些发现将有助于未来的研究,重点关注来曲唑在辅助治疗中的暴露-疗效关系。
