Dosing-time, feeding, and sex-dependent variations of everolimus pharmacokinetics in mice

IF 2.1 4区医学 Q3 PHARMACOLOGY & PHARMACY Fundamental & Clinical Pharmacology Pub Date : 2024-03-18 DOI:10.1111/fcp.13003

Dilek Ozturk Civelek, Narin Ozturk Seyhan, Yasemin Kubra Akyel, Isil Gazioglu, Zeliha Pala Kara, Mehmet N. Orman, Alper Okyar

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Abstract

Background

Everolimus is an oral mammalian target of rapamycin (mTOR) inhibitor used as an immunosuppressant and anticancer. Its pharmacokinetics is highly variable, it has a narrow therapeutic window and shows chronotoxicity with the best time at ZT13 and worst time at ZT1 (ZT; Zeitgeber time, time after light onset) in the preclinical setting.

Objectives

In the present study, we aimed to investigate whether the pharmacokinetics of everolimus vary according to dosing time and whether sex and feeding status interfere with the chronopharmacokinetics.

Method

A single dosage of 5 mg/kg everolimus was administered orally to C57BL/6J male and female mice, in fed or fasted states at ZT1-rest and ZT13-activity times and blood and tissue samples were collected at 0.5, 1, 2, 4, 12, and 24 h following drug administration. Ileum, liver, plasma, and thymus concentrations of everolimus were determined.

Results

Females had a greater ileum AUC_0–24h than males when fed (P = 0.043). Everolimus AUC_0–24h in the liver was substantially greater at ZT1 than at ZT13 in a fasted state (P = 0.001). Plasma C_max, AUC_0–24h, and AUC_total were not statistically significant between the groups (P = 0.098). In one of the target organs of everolimus, the thymus, males had considerably higher amounts at ZT1 than females (P = 0.029).

Conclusion

Our findings imply that the pharmacokinetics of everolimus in mice may differ according to dosing time, sex, and feeding. Greater tissue distribution of everolimus at ZT1 may be associated with the worst tolerated time of everolimus. Our research suggests that oral chronomodulated everolimus therapy may be more effective and safer for cancer patients.

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小鼠依维莫司药代动力学的给药时间、喂食和性别差异。

背景：依维莫司是一种口服哺乳动物雷帕霉素靶标（mTOR）抑制剂，可用作免疫抑制剂和抗癌药。在临床前研究中，它的药代动力学变化很大，治疗窗口很窄，并显示出时间毒性，最佳时间为 ZT13，最差时间为 ZT1（ZT；Zeitgeber 时间，光照开始后的时间）：本研究旨在探讨依维莫司的药代动力学是否会随给药时间的不同而变化，以及性别和喂养状态是否会干扰时间药代动力学：给C57BL/6J雄性和雌性小鼠口服单剂量5 mg/kg依维莫司，分别在ZT1-静息和ZT13-活动时间给药，并在给药后0.5、1、2、4、12和24小时采集血液和组织样本。测定依维莫司在回肠、肝脏、血浆和胸腺中的浓度：结果：喂食时，女性的回肠 AUC0-24h 值高于男性（P = 0.043）。在空腹状态下，肝脏中依维莫司的AUC0-24h在ZT1时比ZT13时要大得多（P = 0.001）。各组间血浆 Cmax、AUC0-24h 和 AUCtotal 的差异无统计学意义（P = 0.098）。在依维莫司的靶器官之一--胸腺中，男性在 ZT1 时的含量明显高于女性（P = 0.029）：我们的研究结果表明，依维莫司在小鼠体内的药代动力学可能因用药时间、性别和喂养方式的不同而不同。依维莫司在 ZT1 阶段的组织分布更广，这可能与依维莫司的最差耐受时间有关。我们的研究表明，对癌症患者来说，口服时间调节型依维莫司疗法可能更有效、更安全。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Fundamental & Clinical Pharmacology 医学-药学

CiteScore

5.30

自引率

6.90%

发文量

111

审稿时长

6-12 weeks

期刊介绍： Fundamental & Clinical Pharmacology publishes reports describing important and novel developments in fundamental as well as clinical research relevant to drug therapy. Original articles, short communications and reviews are published on all aspects of experimental and clinical pharmacology including: Antimicrobial, Antiviral Agents Autonomic Pharmacology Cardiovascular Pharmacology Cellular Pharmacology Clinical Trials Endocrinopharmacology Gene Therapy Inflammation, Immunopharmacology Lipids, Atherosclerosis Liver and G-I Tract Pharmacology Metabolism, Pharmacokinetics Neuropharmacology Neuropsychopharmacology Oncopharmacology Pediatric Pharmacology Development Pharmacoeconomics Pharmacoepidemiology Pharmacogenetics, Pharmacogenomics Pharmacovigilance Pulmonary Pharmacology Receptors, Signal Transduction Renal Pharmacology Thrombosis and Hemostasis Toxicopharmacology Clinical research, including clinical studies and clinical trials, may cover disciplines such as pharmacokinetics, pharmacodynamics, pharmacovigilance, pharmacoepidemiology, pharmacogenomics and pharmacoeconomics. Basic research articles from fields such as physiology and molecular biology which contribute to an understanding of drug therapy are also welcomed.