Determination of Unbound Partition Coefficient and in Vitro-in Vivo Extrapolation for SLC13A Transporter-Mediated Uptake

Riccardi, Keith; Li, Zhenhong; Brown, Janice A.; Gorgoglione, Matthew; Niosi, Mark; Gosset, J; Huard, Kim; Erion, Derek M.; Di, Li

doi:10.1124/dmd.116.071837

Cited by 28 publications

(27 citation statements)

References 20 publications

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“…We have developed a novel experimental approach to predict human clearance for enzyme-and transporter-mediated mechanisms. This method was developed on the basis of liver-to-plasma (Kp uu ) work previously published (Riccardi et al, 2016(Riccardi et al, , 2017. With these hypotheses as a basis: 1) The metabolic, passive, and uptake intrinsic clearance rates in the in vitro hepatocyte assay, in the presence of 4% BSA, are equivalent to in vivo rates, and 2) the metabolic intrinsic clearance rates in the in vitro hepatocyte assay, in the absence of 4% BSA, are equivalent to in vivo rates.…”

Section: Discussionmentioning

confidence: 99%

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A Novel Unified Approach to Predict Human Hepatic Clearance for Both Enzyme- and Transporter-Mediated Mechanisms Using Suspended Human Hepatocytes

et al. 2019

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The accurate prediction of human pharmacokinetics is critically important in modern drug discovery since it drives both pharmacological and toxicological effects. Although significant progress has been made in predicting drug disposition by hepatic drugmetabolizing enzymes, predicting transporter-mediated clearance is still highly uncertain. Furthermore, different approaches are often used to predict clearance with and without transporter involvement, hence the major clearance pathway for a compound must first be determined to know which approach to use. As a result of these challenges, a novel unified method has been developed using cryopreserved suspended human hepatocytes to predict human hepatic clearance for both enzyme-and transporter-mediated mechanisms. This method hypothesizes that, once in vitro metabolic stability is scaled by partition coefficients between hepatocytes and buffer with 4% bovine serum albumin, in vivo clearance can be better predicted. With this method, good in vitro-in vivo correlation of human hepatic clearance has been obtained for a set of 32 structurally diverse compounds, including such transporters as organic anion-transporting polypeptide substrates. The clearance predictions for most compounds are within 3-fold of observed values. This is the first time that multiple compounds result in good in vitro-in vivo extrapolation using an entirely "bottom-up" approach without any empirical scaling factor when transportermediated clearance is involved. Potential exceptions are compounds with significant biliary and/or extra-hepatic clearance. The method offers an alternative approach to more accurately predict human hepatic clearance when multiple complex mechanisms are involved.

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Section: Discussionmentioning

confidence: 99%

“…Presaturation method was also used for highly bound compounds (Riccardi et al, 2015). Calculation of fraction unbound has been discussed previously (Riccardi et al, 2015(Riccardi et al, , 2016(Riccardi et al, , 2017.…”

Section: Methodsmentioning

confidence: 99%

A Novel Unified Approach to Predict Human Hepatic Clearance for Both Enzyme- and Transporter-Mediated Mechanisms Using Suspended Human Hepatocytes

et al. 2019

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“…The f u,cell value was determined by correcting the fraction unbound in homogenate (f u,hom ) by a dilution factor (D) as previously reported (Mateus et al, 2013;Riccardi et al, 2016). Based on a hepatocyte volume of 4 ml for 1 Â 10 6 cells (Reinoso et al, 2001), D was determined to be 25.…”

Section: Discussionmentioning

confidence: 99%

“…time point. K puu,in vitro values can be concentration-dependent (Riccardi et al, 2016), so a follow-up study was performed in which the cell and medium concentrations were measured following incubation with the full range of inducer concentrations for 24 hours. The K puu,in vitro values decreased as the nominal concentrations of bosentan and rifampicin increased ( Fig.…”

Section: Lotmentioning

confidence: 99%

“…To date, numerous methods have been proposed for determining intracellular unbound concentrations of drugs; however, as highlighted in a recent white paper, no systematic evaluation has been conducted to determine which method is the most reliable (Ulvestad et al, 2011;Zhu et al, 2014). Estimation of the f u,cell using cell homogenate has been widely used in recent years (Mateus et al, 2013;Chien et al, 2016;Riccardi et al, 2016). Furthermore, the K puu,in vitro values estimated using this method were reported to be in agreement with the fold difference in IC 50 estimated in human liver microsomes versus cell lines, providing confidence in the estimated f u,cell (Riccardi et al, 2016).…”

Section: Downloaded Frommentioning

confidence: 99%

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Quantitative Prediction of CYP3A4 Induction: Impact of Measured, Free, and Intracellular Perpetrator Concentrations from Human Hepatocyte Induction Studies on Drug-Drug Interaction Predictions

et al. 2017

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Typically, concentration-response curves are based upon nominal inducer concentrations for in-vitro-to-in-vivo extrapolation of CYP3A4 induction. The limitation of this practice is that it assumes the hepatocyte culture model is a static system. We assessed whether correcting for: 1) changes in perpetrator concentration in the induction medium during the incubation period, 2) perpetrator binding to proteins in the induction medium, and 3) nonspecific binding of perpetrator can improve the accuracy of CYP3A4 induction predictions. Of the seven compounds used in this evaluation, significant parent loss and nonspecific binding were observed for rifampicin (29.3-38.3%), pioglitazone (64.3-78.6%), and rosiglitazone (57.1-75.5%). As a result, the free measured EC values (EC) of pioglitazone, rosiglitazone, and rifampicin were significantly lower than the nominal EC values. In general, the accuracy of the induction predictions, using multiple static models, improved when corrections were made for measured medium concentrations, medium protein binding, and nonspecific binding of the perpetrator, as evidenced by 18-29% reductions in the root mean square error. The relative induction score model performed better than the basic static and mechanistic static models, resulting in lower prediction error and no false-positive or false-negative predictions. However, even when the EC value was used, the induction prediction for bosentan, which is a substrate of organic anion transporter proteins, was overpredicted by approximately 2-fold. Accounting for the ratio of unbound intracellular concentrations to unbound medium concentrations (K) (0.5-7.5) and the predicted multiple-dose K (0.6) for bosentan resulted in induction predictions within 35% of the observed interaction.

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Determination of Fraction Unbound and Unbound Partition Coefficient to Estimate Intracellular Free Drug Concentration

Ryu

Riccardi

Jordan

et al. 2021

Methods in Pharmacology and Toxicology

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Determination of Unbound Partition Coefficient and in Vitro-in Vivo Extrapolation for SLC13A Transporter-Mediated Uptake

Cited by 28 publications

References 20 publications

A Novel Unified Approach to Predict Human Hepatic Clearance for Both Enzyme- and Transporter-Mediated Mechanisms Using Suspended Human Hepatocytes

A Novel Unified Approach to Predict Human Hepatic Clearance for Both Enzyme- and Transporter-Mediated Mechanisms Using Suspended Human Hepatocytes

Quantitative Prediction of CYP3A4 Induction: Impact of Measured, Free, and Intracellular Perpetrator Concentrations from Human Hepatocyte Induction Studies on Drug-Drug Interaction Predictions

Determination of Fraction Unbound and Unbound Partition Coefficient to Estimate Intracellular Free Drug Concentration

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