Hsing-Chieh Lin , Courtney Sakolish , Haley L. Moyer , Paul L. Carmichael , Maria T. Baltazar , Stephen S. Ferguson , Jason P. Stanko , Philip Hewitt , Ivan Rusyn , Weihsueh A. Chiu
{"title":"预测全氟辛烷磺酸肾清除率的体外-硅学工作流程。","authors":"Hsing-Chieh Lin , Courtney Sakolish , Haley L. Moyer , Paul L. Carmichael , Maria T. Baltazar , Stephen S. Ferguson , Jason P. Stanko , Philip Hewitt , Ivan Rusyn , Weihsueh A. Chiu","doi":"10.1016/j.taap.2024.117015","DOIUrl":null,"url":null,"abstract":"<div><p><em>Per</em>- and poly-fluoroalkyl substances (PFAS) have a wide range of elimination half-lives (days to years) in humans, thought to be in part due to variation in proximal tubule reabsorption. While human biomonitoring studies provide important data for some PFAS, renal clearance (CL<sub>renal</sub>) predictions for hundreds of PFAS in commerce requires experimental studies with <em>in vitro</em> models and physiologically-based <em>in vitro</em>-to-<em>in vivo</em> extrapolation (IVIVE). Options for studying renal proximal tubule pharmacokinetics include cultures of renal proximal tubule epithelial cells (RPTECs) and/or microphysiological systems. This study aimed to compare CL<sub>renal</sub> predictions for PFAS using <em>in vitro</em> models of varying complexity (96-well plates, static 24-well Transwells and a fluidic microphysiological model, all using human telomerase reverse transcriptase-immortalized and OAT1-overexpressing RPTECs combined with <em>in silico</em> physiologically-based IVIVE. Three PFAS were tested: one with a long half-life (PFOS) and two with shorter half-lives (PFHxA and PFBS). PFAS were added either individually (5 μM) or as a mixture (2 μM of each substance) for 48 h. Bayesian methods were used to fit concentrations measured in media and cells to a three-compartmental model to obtain the <em>in vitro</em> permeability rates, which were then used as inputs for a physiologically-based IVIVE model to estimate <em>in vivo</em> CL<sub>renal</sub>. Our predictions for human CL<sub>renal</sub> of PFAS were highly concordant with available values from <em>in vivo</em> human studies. The relative values of CL<sub>renal</sub> between slow- and faster-clearance PFAS were most highly concordant between predictions from 2D culture and corresponding <em>in vivo</em> values. However, the predictions from the more complex model (with or without flow) exhibited greater concordance with absolute CL<sub>renal</sub>. Overall, we conclude that a combined <em>in vitro-in silico</em> workflow can predict absolute CL<sub>renal</sub> values, and effectively distinguish between PFAS with slow and faster clearance, thereby allowing prioritization of PFAS with a greater potential for bioaccumulation in humans.</p></div>","PeriodicalId":23174,"journal":{"name":"Toxicology and applied pharmacology","volume":null,"pages":null},"PeriodicalIF":3.3000,"publicationDate":"2024-06-23","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"An in vitro-in silico workflow for predicting renal clearance of PFAS\",\"authors\":\"Hsing-Chieh Lin , Courtney Sakolish , Haley L. Moyer , Paul L. Carmichael , Maria T. Baltazar , Stephen S. Ferguson , Jason P. Stanko , Philip Hewitt , Ivan Rusyn , Weihsueh A. Chiu\",\"doi\":\"10.1016/j.taap.2024.117015\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><p><em>Per</em>- and poly-fluoroalkyl substances (PFAS) have a wide range of elimination half-lives (days to years) in humans, thought to be in part due to variation in proximal tubule reabsorption. While human biomonitoring studies provide important data for some PFAS, renal clearance (CL<sub>renal</sub>) predictions for hundreds of PFAS in commerce requires experimental studies with <em>in vitro</em> models and physiologically-based <em>in vitro</em>-to-<em>in vivo</em> extrapolation (IVIVE). Options for studying renal proximal tubule pharmacokinetics include cultures of renal proximal tubule epithelial cells (RPTECs) and/or microphysiological systems. This study aimed to compare CL<sub>renal</sub> predictions for PFAS using <em>in vitro</em> models of varying complexity (96-well plates, static 24-well Transwells and a fluidic microphysiological model, all using human telomerase reverse transcriptase-immortalized and OAT1-overexpressing RPTECs combined with <em>in silico</em> physiologically-based IVIVE. Three PFAS were tested: one with a long half-life (PFOS) and two with shorter half-lives (PFHxA and PFBS). PFAS were added either individually (5 μM) or as a mixture (2 μM of each substance) for 48 h. Bayesian methods were used to fit concentrations measured in media and cells to a three-compartmental model to obtain the <em>in vitro</em> permeability rates, which were then used as inputs for a physiologically-based IVIVE model to estimate <em>in vivo</em> CL<sub>renal</sub>. Our predictions for human CL<sub>renal</sub> of PFAS were highly concordant with available values from <em>in vivo</em> human studies. The relative values of CL<sub>renal</sub> between slow- and faster-clearance PFAS were most highly concordant between predictions from 2D culture and corresponding <em>in vivo</em> values. However, the predictions from the more complex model (with or without flow) exhibited greater concordance with absolute CL<sub>renal</sub>. 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An in vitro-in silico workflow for predicting renal clearance of PFAS
Per- and poly-fluoroalkyl substances (PFAS) have a wide range of elimination half-lives (days to years) in humans, thought to be in part due to variation in proximal tubule reabsorption. While human biomonitoring studies provide important data for some PFAS, renal clearance (CLrenal) predictions for hundreds of PFAS in commerce requires experimental studies with in vitro models and physiologically-based in vitro-to-in vivo extrapolation (IVIVE). Options for studying renal proximal tubule pharmacokinetics include cultures of renal proximal tubule epithelial cells (RPTECs) and/or microphysiological systems. This study aimed to compare CLrenal predictions for PFAS using in vitro models of varying complexity (96-well plates, static 24-well Transwells and a fluidic microphysiological model, all using human telomerase reverse transcriptase-immortalized and OAT1-overexpressing RPTECs combined with in silico physiologically-based IVIVE. Three PFAS were tested: one with a long half-life (PFOS) and two with shorter half-lives (PFHxA and PFBS). PFAS were added either individually (5 μM) or as a mixture (2 μM of each substance) for 48 h. Bayesian methods were used to fit concentrations measured in media and cells to a three-compartmental model to obtain the in vitro permeability rates, which were then used as inputs for a physiologically-based IVIVE model to estimate in vivo CLrenal. Our predictions for human CLrenal of PFAS were highly concordant with available values from in vivo human studies. The relative values of CLrenal between slow- and faster-clearance PFAS were most highly concordant between predictions from 2D culture and corresponding in vivo values. However, the predictions from the more complex model (with or without flow) exhibited greater concordance with absolute CLrenal. Overall, we conclude that a combined in vitro-in silico workflow can predict absolute CLrenal values, and effectively distinguish between PFAS with slow and faster clearance, thereby allowing prioritization of PFAS with a greater potential for bioaccumulation in humans.
期刊介绍:
Toxicology and Applied Pharmacology publishes original scientific research of relevance to animals or humans pertaining to the action of chemicals, drugs, or chemically-defined natural products.
Regular articles address mechanistic approaches to physiological, pharmacologic, biochemical, cellular, or molecular understanding of toxicologic/pathologic lesions and to methods used to describe these responses. Safety Science articles address outstanding state-of-the-art preclinical and human translational characterization of drug and chemical safety employing cutting-edge science. Highly significant Regulatory Safety Science articles will also be considered in this category. Papers concerned with alternatives to the use of experimental animals are encouraged.
Short articles report on high impact studies of broad interest to readers of TAAP that would benefit from rapid publication. These articles should contain no more than a combined total of four figures and tables. Authors should include in their cover letter the justification for consideration of their manuscript as a short article.
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