中文English
ISSN 1001-5256 (Print)
ISSN 2097-3497 (Online)
CN 22-1108/R
Volume 41 Issue 9
Sep.  2025
Turn off MathJax
Article Contents
Article Navigation >  Journal of Clinical Hepatology  > 2025  >  41(9): 1853-1860

Pharmacokinetic interactions between empagliflozin and donafenib/lenvatinib in rats

DOI: 10.12449/JCH250921

  • Department of Pharmacy,Hebei Key Laboratory of Clinical Pharmacy,Hebei General Hospital,Shijiazhuang 050017,China

Research funding:

Natural Science Foundation of Hebei Province (H2022307063);

Medical Science Research Project of Hebei (20250297)

More Information
  • Corresponding author: DONG Zhanjun, 13313213656@126.com (ORCID: 0000-0001-5349-4970)
  • Received Date: 2025-03-11
  • Accepted Date: 2025-05-15
  • Published Date: 2025-09-25
    Abstract
  •   Objective  To investigate the influence of empagliflozin combined with donafenib or lenvatinib on the pharmacokinetic parameters of each drug, and to provide a reference for combined medication in clinical practice.  Methods  A total of 48 healthy male Sprague-Dawley rats were divided into 8 groups: empagliflozin group 1 and 2, donafenib group, lenvatinib group, donafenib pretreatment+empagliflozin group, lenvatinib pretreatment + empagliflozin group, empagliflozin pretreatment+donafenib group, and empagliflozin pretreatment+lenvatinib group, with 6 rats in each group. The doses of empagliflozin, donafenib, and lenvatinib were 2.5 mg/kg, 40 mg/kg, and 1.2 mg/kg, respectively. The rats in the empagliflozin group, donafenib group, and lenvatinib group were given a blank solvent by gavage for 7 consecutive days, followed by a single dose of empagliflozin, donafenib, or lenvatinib on day 7 after the administration of the blank solvent; the rats in the pretreatment groups were given the pretreatment drug by gavage for 7 consecutive days, followed by a single dose of drug combination on day 7 after administration of the pretreatment drug. Blood samples were collected at different time points, and plasma was separated to measure the concentration of each drug. A validated ultra-performance liquid chromatography-tandem mass spectrometry method was used to measure the plasma concentrations of donafenib, lenvatinib, and empagliflozin, and a non-compartmental model was used to calculate the main pharmacokinetic parameters of each drug (area under the plasma concentration-time curve [AUC], time to peak [Tmax], peak concentration [Cmax], and half-life time [t1/2]). The independent-samples t test was used for comparison of normally distributed continuous data between two groups, and the Mann-Whitney U test was used for comparison of non-normally distributed continuous data between two groups.  Results  Compared with the empagliflozin group, the donafenib pretreatment+empagliflozin group had significant increases in the AUC0-t and AUC0-∞ of empagliflozin (P=0.011 and 0.008), while the lenvatinib pretreatment+empagliflozin group had no significant change in the AUC of empagliflozin, with a slightly shorter TmaxP=0.019). Compared with the donafenib group, the empagliflozin pretreatment+donafenib group had significant increases in the AUC0-t and AUC0-∞ of donafenib (P=0.027 and 0.025), as well as a significant increase in CmaxP=0.015) and significant reductions in CLz/F and Vz/FP=0.005 and 0.004); compared with the lenvatinib group, the empagliflozin pretreatment+lenvatinib group had a reduction in the t1/2 of lenvatinib by approximately 5 hours (P=0.002), with a trend of reduction in AUC0-tP>0.05).  Conclusion  Empagliflozin combined with donafenib may alter the pharmacokinetic parameters of both drugs, leading to a significant increase in the exposure levels of both drugs, and efficacy and adverse reactions should be monitored during co-administration. There are no significant changes in the exposure levels of empagliflozin and lenvatinib during co-administration.

     

    • FullText(HTML)
  • loading
    • References(18)
  • [1]
    SCOTT LJ. Lenvatinib: First global approval[J]. Drugs, 2015, 75( 5): 553- 560. DOI: 10.1007/s40265-015-0383-0.
    [2]
    GUPTA A, JARZAB B, CAPDEVILA J, et al. Population pharmacokinetic analysis of lenvatinib in healthy subjects and patients with cancer[J]. Br J Clin Pharmacol, 2016, 81( 6): 1124- 1133. DOI: 10.1111/bcp.12907.
    [3]
    HE XR, LI Y, LI YJ, et al. In vivo assessment of the pharmacokinetic interactions between donafenib and dapagliflozin, donafenib and canagliflozin in rats[J]. Biomed Pharmacother, 2023, 162: 114663. DOI: 10.1016/j.biopha.2023.114663.
    [4]
    MIRARCHI L, AMODEO S, CITARRELLA R, et al. SGLT2 inhibitors as the most promising influencers on the outcome of non-alcoholic fatty liver disease[J]. Int J Mol Sci, 2022, 23( 7): 3668. DOI: 10.3390/ijms23073668.
    [5]
    LIU ZH, DU WY, GUO CH, et al. Research progress of empagliflozin in the treatment of type 2 diabe-tes mellitus and cardiovascular and renal benefits[J]. Chin J Clin Pharmacol Ther, 2025, 30( 3): 412- 418. DOI: 10.12092/j.issn.1009-2501.2025.03.015.

    刘子涵, 杜文雨, 郭彩会, 等. 恩格列净治疗2型糖尿病和心肾获益的研究进展[J]. 中国临床药理学与治疗学, 2025, 30( 3): 412- 418. DOI: 10.12092/j.issn.1009-2501.2025.03.015.
    [6]
    STÖLLBERGER C, FINSTERER J, SCHNEIDER B. Adverse events and drug-drug interactions of sodium glucose co-transporter 2 inhibitors in patients treated for heart failure[J]. Expert Rev Cardiovasc Ther, 2023, 21( 11): 803- 816. DOI: 10.1080/14779072.2023.2273900.
    [7]
    CUI YJ, LI Y, FAN LJ, et al. UPLC-MS/MS method for the determination of Lenvatinib in rat plasma and its application to drug-drug interaction studies[J]. J Pharm Biomed Anal, 2021, 206: 114360. DOI: 10.1016/j.jpba.2021.114360.
    [8]
    Chinese Pharmacopoeia Committee. Pharmacopoeia of People’s Republic of China(PRC)-part IV(2020 edition)[M]. Beijing: China Medical Science Press, 2020.

    国家药典委员会. 中华人民共和国药典-四部(2020年版)[M]. 北京: 中国医药科技出版社, 2020.
    [9]
    SCHEEN AJ. Pharmacokinetic and pharmacodynamic profile of empagliflozin, a sodium glucose co-transporter 2 inhibitor[J]. Clin Pharmacokinet, 2014, 53( 3): 213- 225. DOI: 10.1007/s40262-013-0126-x.
    [10]
    GARCIA-ROPERO A, BADIMON JJ, SANTOS-GALLEGO CG. The pharmacokinetics and pharmacodynamics of SGLT2 inhibitors for type 2 diabetes mellitus: The latest developments[J]. Expert Opin Drug Metab Toxicol, 2018, 14( 12): 1287- 1302. DOI: 10.1080/17425255.2018.1551877.
    [11]
    KEAM SJ, DUGGAN S. Donafenib: First approval[J]. Drugs, 2021, 81( 16): 1915- 1920. DOI: 10.1007/s40265-021-01603-0.
    [12]
    REAGAN-SHAW S, NIHAL M, AHMAD N. Dose translation from animal to human studies revisited[J]. FASEB J, 2008, 22( 3): 659- 661. DOI: 10.1096/fj.07-9574LSF.
    [13]
    MACHA S, KOENEN R, SENNEWALD R, et al. Effect of gemfibrozil, rifampicin, or probenecid on the pharmacokinetics of the SGLT2 inhibitor empagliflozin in healthy volunteers[J]. Clin Ther, 2014, 36( 2): 280- 290. e 1. DOI: 10.1016/j.clinthera.2014.01.003.
    [14]
    DENG YR, CAO GX, YAN B, et al. Effect of sorafenib and donafenib on the pharmacokinetics of ertugliflozin in rats[J]. J Clin Hepatol, 2025, 41( 1): 92- 98. DOI: 10.12449/JCH250114.

    邓艳茹, 曹格溪, 闫彬, 等. 索拉非尼和多纳非尼对大鼠体内艾托格列净药代动力学的影响[J]. 临床肝胆病杂志, 2025, 41( 1): 92- 98. DOI: 10.12449/JCH250114.
    [15]
    WANG XM, ZHANG X, HUANG XH, et al. The drug-drug interaction of sorafenib mediated by P-glycoprotein and CYP3A4[J]. Xenobiotica, 2016, 46( 7): 651- 658. DOI: 10.3109/00498254.2015.1109160.
    [16]
    LI JM, WANG XQ, NING C, et al. Influences of ABC transporter and CYP3A4/5 genetic polymorphisms on the pharmacokinetics of lenvatinib in Chinese healthy subjects[J]. Eur J Clin Pharmacol, 2020, 76( 8): 1125- 1133. DOI: 10.1007/s00228-020-02879-z.
    [17]
    SHUMAKER R, ALURI J, FAN J, et al. Effects of ketoconazole on the pharmacokinetics of lenvatinib(E7080) in healthy participants[J]. Clin Pharmacol Drug Dev, 2015, 4( 2): 155- 160. DOI: 10.1002/cpdd.140.
    [18]
    SHUMAKER RC, ALURI J, FAN J, et al. Effect of rifampicin on the pharmacokinetics of lenvatinib in healthy adults[J]. Clin Drug Investig, 2014, 34( 9): 651- 659. DOI: 10.1007/s40261-014-0217-y.
    • Relative Articles
    • Supplements(0)
    • Cited By
  • 加载中

Catalog

    通讯作者: 陈斌, bchen63@163.com
    • 1. 

      沈阳化工大学材料科学与工程学院 沈阳 110142

    1. 本站搜索
    2. 百度学术搜索
    3. 万方数据库搜索
    4. CNKI搜索

    Figures(4)  / Tables(7)

    Get Citation
    PDF
    XML

    Article Metrics

    Article views (95) PDF downloads(9) Cited by()
    Proportional views
    Related
        

    The first journal specializing in hepatobiliary and pancreatic diseases in China

    Supervisor:Ministry of Education of the People's Republic of China

    Sponsor:Jilin University

    Academic Support: Chinese Society of Hepatology,Chinese Medical Association

    Address: 461 Xinjiang Road, Changchun

    Submit:0431-88782044

    Peer review:0431-88783542

    Email:lcgdb@vip.163.com

    About Journal

    Submission Guideline

    Journal Online

    Hepatobiliary College

    Guidelines

    YesterdayIP[]YesterdayPV[]TodayIP[]TodayPV[]Online[]

    Website Design © 2020 Editorial Board of Journal of Clinical Hepatology 吉ICP备10000617号-1 Supported by: Beijing Renhe Information Technology Co. Ltd  

    /

    DownLoad:  Full-Size Img  PowerPoint
    Return
    Return