Mathematical Modeling of the <i>in Vitro</i> Hepatic Disposition of Mycophenolic Acid and Its Glucuronide in Sandwich-Cultured Human Hepatocytes

Matsunaga, Norikazu; Wada, Shintaro; Nakanishi, Takeo; Ikenaga, Miho; Ogawa, Michio; Tamai, Ikumi

doi:10.1021/mp400513k

Cited by 25 publications

(29 citation statements)

References 51 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Recently, Pfeifer et al (2013a,b) and Matsunaga et al (2014) demonstrated the importance of the interplay between basolateral and canalicular efflux in the systemic and hepatic disposition of rosuvastatin and mycophenolic acid glucuronide, respectively. Extensive biliary excretion of rosuvastatin and mycophenolic acid glucuronide required mathematical modeling to deconvolute the contribution of basolateral versus canalicular transport.…”

Section: Discussionmentioning

confidence: 99%

Role of Multidrug Resistance–Associated Protein 4 in the Basolateral Efflux of Hepatically Derived Enalaprilat

et al. 2014

View full text Add to dashboard Cite

Hepatic uptake and efflux transporters govern the systemic and hepatic exposure of many drugs and metabolites. Enalapril is a pharmacologically inactive prodrug of enalaprilat. Following oral administration, enalapril is converted to enalaprilat in hepatocytes and undergoes translocation into the systemic circulation to exert its pharmacologic effect by inhibiting angiotensin-converting enzyme. Although the transport proteins governing hepatic uptake of enalapril and the biliary excretion of enalapril and enalaprilat are well established, it remains unknown how hepatically derived enalaprilat translocates across the basolateral membrane into the systemic circulation. In this study, the role of ATP-binding cassette transporters in the hepatic basolateral efflux of enalaprilat was investigated using membrane vesicles. ATP-dependent uptake of enalaprilat into vesicles expressing multidrug resistance-associated protein (MRP) 4 was significantly greater (∼3.8-fold) than in control vesicles. In contrast, enalaprilat was not transported to a significant extent by MRP3, and enalapril was not transported by either MRP3 or MRP4. The functional importance of MRP4 in the basolateral excretion of derived enalaprilat was evaluated using a novel basolateral efflux protocol developed in human sandwich-cultured hepatocytes. Under normal culture conditions, the mean intrinsic basolateral efflux clearance (CL int,basolateral ) of enalaprilat was 0.026 6 0.012 ml/min; enalaprilat CL int,basolateral was significantly reduced to 0.009 6 0.009 ml/min by pretreatment with the pan-MRP inhibitor MK-571. Results suggest that hepatically derived enalaprilat is excreted across the hepatic basolateral membrane by MRP4. Changes in MRP4-mediated basolateral efflux may alter the systemic concentrations of this active metabolite, and potentially the efficacy of enalapril.

show abstract

Section: Discussionmentioning

confidence: 99%

Role of Multidrug Resistance–Associated Protein 4 in the Basolateral Efflux of Hepatically Derived Enalaprilat

et al. 2014

View full text Add to dashboard Cite

show abstract

“…Cryopreserved human hepatocytes were thawed, plated, and cultured as described in our previous study (Matsunaga et al, 2014), and human SCHs on day 4 were used. Modulation of Ca 2+ in the incubation buffer was applied to maintain or disrupt the canalicular networks between cells sealed by tight junctions.…”

Section: Methodsmentioning

confidence: 99%

“…Using this approach, the masses of compounds in the bile canalicular lumen can be measured with Ca 2+ -containing and Ca 2+ -free buffers (B-CLEAR technology; Qualyst Transporter Solutions, Durham, NC) (Brouwer et al, 2013). Metabolism and hepatobiliary transport studies of human SCHs were performed as described in our previous report (Matsunaga et al, 2014). In brief, human SCHs were incubated with Ca 2+ -containing or Ca 2+ -free buffer containing bosentan at an initial concentration of 1 mM at 37°C for 3, 5, 10, 15, 20, 30, or 45 minutes.…”

Section: Methodsmentioning

confidence: 99%

“…Furthermore, model-based concepts have recently become widespread in various research fields, including drug discovery and development. Several model-based analyses have been undertaken for the hepatic disposition of drugs and their metabolites in human SCHs to predict intracellular concentration changes by alterations in hepatobiliary transport, to investigate rate-limiting transport processes, and to evaluate drug-drug interaction at clinically relevant concentrations (Lee et al, 2010;Matsunaga et al, 2014Matsunaga et al, , 2015.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Analysis of the Metabolic Pathway of Bosentan and of the Cytotoxicity of Bosentan Metabolites Based on a Quantitative Modeling of Metabolism and Transport in Sandwich-Cultured Human Hepatocytes

Matsunaga

Kaneko

Staub

et al. 2015

Drug Metabolism and Disposition

View full text Add to dashboard Cite

To quantitatively understand the events in the human liver, we modeled a hepatic disposition of bosentan and its three known metabolites (Ro 48-5033, Ro 47-8634, and Ro 64-1056) in sandwichcultured human hepatocytes based on the known metabolic pathway. In addition, the hepatotoxicity of Ro 47-8634 and Ro 64-1056 was investigated because bosentan is well known as a hepatotoxic drug. A model illustrating the hepatic disposition of bosentan and its three metabolites suggested the presence of a novel metabolic pathway(s) from the three metabolites. By performing in vitro metabolism studies on human liver microsomes, a novel metabolite (M4) was identified in Ro 47-8634 metabolism, and its structure was determined. Moreover, by incorporating the metabolic pathway of Ro 47-8634 to M4 into the model, the hepatic disposition of bosentan and its three metabolites was successfully estimated. In hepatocyte toxicity studies, the cell viability of human hepatocytes decreased after exposure to Ro 47-8634, and the observed hepatotoxicity was diminished by pretreatment with tienilic acid (CYP2C9-specific inactivator). Pretreatment with 1-aminobenzotriazole (broad cytochrome P450 inactivator) also tended to maintain the cell viability. Furthermore, Ro 64-1056 showed hepatotoxicity in a concentrationdependent manner. These results suggest that Ro 64-1056 is directly involved in bosentan-induced liver injury partly because CYP2C9 specifically mediates hydroxylation of the t-butyl group of Ro 47-8634. Our findings demonstrate the usefulness of a quantitative modeling of hepatic disposition of drugs and metabolites in sandwichcultured hepatocytes. In addition, the newly identified metabolic pathway may be an alternative route that can avoid Ro 64-1056-induced liver injury.

show abstract

“…To overcome this limitation, mechanistic pharmacokinetic modeling coupled with data from sandwichcultured hepatocytes has been used to deconvolute the relative contribution of various clearance (CL) pathways to the disposition of rosuvastatin, mycophenolic acid, and 3 H-taurocholic acid (TCA) (Pfeifer et al, 2013c;Matsunaga et al, 2014;Yang et al, 2015). Transporters are expressed and properly localized in the sandwich-cultured hepatocyte system, which can be used to assess the function of multiple transporters (Yang et al, 2016).…”

Section: Introductionmentioning

confidence: 99%

Prediction of Altered Bile Acid Disposition Due to Inhibition of Multiple Transporters: An Integrated Approach Using Sandwich-Cultured Hepatocytes, Mechanistic Modeling, and Simulation

Guo

Yang

Brouwer

et al. 2016

Journal of Pharmacology and Experimental Therapeutics

View full text Add to dashboard Cite

Transporter-mediated alterations in bile acid disposition may have significant toxicological implications. Current methods to predict interactions are limited by the interplay of multiple transporters, absence of protein in the experimental system, and inaccurate estimates of inhibitor concentrations. An integrated approach was developed to predict altered bile acid disposition due to inhibition of multiple transporters using the model bile acid taurocholate (TCA). TCA pharmacokinetic parameters were estimated by mechanistic modeling using sandwich-cultured human hepatocyte data with protein in the medium. Uptake, basolateral efflux, and biliary clearance estimates were 0.63, 0.034, and 0.074 mL/min/g liver, respectively. Cellular total TCA concentrations (C t,Cells ) were selected as the model output based on sensitivity analysis. Monte Carlo simulations of TCA C t,Cells in the presence of model inhibitors (telmisartan and bosentan) were performed using inhibition constants for TCA transporters and inhibitor concentrations, including cellular total inhibitor concentrations ([I] t,cell ) or unbound concentrations, and cytosolic total or unbound concentrations. For telmisartan, the model prediction was accurate with an average fold error (AFE) of 0.99-1.0 when unbound inhibitor concentration ([I] u ) was used; accuracy dropped when total inhibitor concentration ([I] t ) was used. For bosentan, AFE was 1.2-1.3 using either [I] u or [I] t . This difference was evaluated by sensitivity analysis of the cellular unbound fraction of inhibitor (f u,cell,inhibitor ), which revealed higher sensitivity of f u,cell,inhibitor for predicting TCA C t,Cells when inhibitors exhibited larger ([I] t,cell /IC 50 ) values. In conclusion, this study demonstrated the applicability of a framework to predict hepatocellular bile acid concentrations due to drug-mediated inhibition of transporters using mechanistic modeling and cytosolic or cellular unbound concentrations.

show abstract

Mathematical Modeling of the in Vitro Hepatic Disposition of Mycophenolic Acid and Its Glucuronide in Sandwich-Cultured Human Hepatocytes

Cited by 25 publications

References 51 publications

Role of Multidrug Resistance–Associated Protein 4 in the Basolateral Efflux of Hepatically Derived Enalaprilat

Role of Multidrug Resistance–Associated Protein 4 in the Basolateral Efflux of Hepatically Derived Enalaprilat

Analysis of the Metabolic Pathway of Bosentan and of the Cytotoxicity of Bosentan Metabolites Based on a Quantitative Modeling of Metabolism and Transport in Sandwich-Cultured Human Hepatocytes

Prediction of Altered Bile Acid Disposition Due to Inhibition of Multiple Transporters: An Integrated Approach Using Sandwich-Cultured Hepatocytes, Mechanistic Modeling, and Simulation

Contact Info

Product

Resources

About