OAT3 Participates in Drug–Drug Interaction between Bentysrepinine and Entecavir through Interactions with M8—A Metabolite of Bentysrepinine—In Rats and Humans In Vitro

Zhang, Aijie; Yang, Fan-Long; Yang, Yuan; Li, Cai; Huo, Xiaokui; Liu, Jing; Zhou, Shenzhi; Li, Wei; Zhang, Na; Liu, Jianfeng; Su, Dong; Fan, Huirong; Peng, Ying; Zheng, Jiang

doi:10.3390/molecules28041995

Cited by 2 publications

(1 citation statement)

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“…Zhang et al conducted pharmacokinetic studies and uptake assays using rat renal slices and hOAT1/3-HEK293 cells to assess the potential DDI between bentysrepinine and entecavir. The study results led to the conclusion that it is safe to use bentysrepinine with entecavir in clinical practice [ 102 ]. Xu, Q. et al utilized LC-MS/MS to determine the plasma and urine concentrations of entecavir after intravenous and oral administration in vivo, as well as assess entecavir uptake in kidney slices and transfected cells in vitro.…”

Section: Methods For the Study Of Ddis Mediated By Renal Transportersmentioning

confidence: 99%

Research Methods and New Advances in Drug–Drug Interactions Mediated by Renal Transporters

et al. 2023

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The kidney is critical in the human body’s excretion of drugs and their metabolites. Renal transporters participate in actively secreting substances from the proximal tubular cells and reabsorbing them in the distal renal tubules. They can affect the clearance rates (CLr) of drugs and their metabolites, eventually influence the clinical efficiency and side effects of drugs, and may produce drug–drug interactions (DDIs) of clinical significance. Renal transporters and renal transporter-mediated DDIs have also been studied by many researchers. In this article, the main types of in vitro research models used for the study of renal transporter-mediated DDIs are membrane-based assays, cell-based assays, and the renal slice uptake model. In vivo research models include animal experiments, gene knockout animal models, positron emission tomography (PET) technology, and studies on human beings. In addition, in vitro–in vivo extrapolation (IVIVE), ex vivo kidney perfusion (EVKP) models, and, more recently, biomarker methods and in silico models are included. This article reviews the traditional research methods of renal transporter-mediated DDIs, updates the recent progress in the development of the methods, and then classifies and summarizes the advantages and disadvantages of each method. Through the sorting work conducted in this paper, it will be convenient for researchers at different learning stages to choose the best method for their own research based on their own subject’s situation when they are going to study DDIs mediated by renal transporters.

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Section: Methods For the Study Of Ddis Mediated By Renal Transportersmentioning

confidence: 99%