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Interplay of Ritonavir-Boosted Oral Cabazitaxel with the Organic Anion-Transporting Polypeptide (OATP) Uptake Transporters and Carboxylesterase 1 in Mice

有机阴离子转运多肽 利托那韦 羧酸酯酶 化学 有机阴离子转运蛋白1 运输机 药理学 硝化酶 生物化学 生物 基因 病毒学 病毒载量 抗逆转录病毒疗法 人类免疫缺陷病毒(HIV)
作者
Nancy H.C. Loos,Margarida L.F. Martins,Jamie Rijmers,Daniëlle de Jong,Maria C. Lebre,Matthijs M. Tibben,Jos H. Beijnen,Alfred H. Schinkel
出处
期刊:Molecular Pharmaceutics [American Chemical Society]
卷期号:21 (4): 1952-1964
标识
DOI:10.1021/acs.molpharmaceut.3c01205
摘要

Intravenously administered chemotherapeutic cabazitaxel is used for palliative treatment of prostate cancer. An oral formulation would be more patient-friendly and reduce the need for hospitalization. We therefore study determinants of the oral pharmacokinetics of cabazitaxel in a ritonavir-boosted setting, which reduces the CYP3A-mediated first-pass metabolism of cabazitaxel. We here assessed the role of organic anion-transporting polypeptides (OATPs) in the disposition of orally boosted cabazitaxel and its active metabolites, using the Oatp1a/b-knockout and the OATP1B1/1B3-transgenic mice. These transporters may substantially affect plasma clearance and hepatic and intestinal drug disposition. The pharmacokinetics of cabazitaxel and DM2 were not significantly affected by Oatp1a/b and OATP1B1/1B3 activity. In contrast, the plasma AUC0–120 min of DM1 in Oatp1a/b–/– was 1.9-fold (p < 0.05) higher than that in wild-type mice, and that of docetaxel was 2.4-fold (p < 0.05) higher. We further observed impaired hepatic uptake and intestinal disposition for DM1 and docetaxel in the Oatp-ablated strains. None of these parameters showed rescue by the OATP1B1 or -1B3 transporters in the humanized mouse strains, suggesting a minimal role of OATP1B1/1B3. Ritonavir itself was also a potent substrate for mOatp1a/b, showing a 2.9-fold (p < 0.0001) increased plasma AUC0–120 min and 3.5-fold (p < 0.0001) decreased liver-to-plasma ratio in Oatp1a/b–/– compared to those in wild-type mice. Furthermore, we observed the tight binding of cabazitaxel and its active metabolites, including docetaxel, to plasma carboxylesterase (Ces1c) in mice, which may complicate the interpretation of pharmacokinetic and pharmacodynamic mouse studies. Collectively, these results will help to further optimize (pre)clinical research into the safety and efficacy of orally applied cabazitaxel.
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