2002
DOI: 10.1124/dmd.30.8.892
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Prediction of Hepatic Clearance and Availability by Cryopreserved Human Hepatocytes: An Application of Serum Incubation Method

Abstract: ABSTRACT:A novel and convenient method was established for the prediction of in vivo metabolic clearance in human liver. The present method applied the in vitro-in vivo extrapolation paradigm previously established in rats to the in vitro data obtained from cryopreserved human hepatocytes. Predicted hepatic availability and clearance were compared with the reported oral bioavailability and plasma clearance in humans for 14 clinically used drugs (naloxone, buspirone, verapamil, lidocaine, imipramine, metoprolol… Show more

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Cited by 157 publications
(168 citation statements)
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“…CL int, in vivo data were provided in several reports (Shibata et al, 2002;Naritomi et al, 2003). Relationships obtained using the parallel tube model to compute CL int, in vivo were very similar to those reported (data not shown).…”
Section: Methodssupporting
confidence: 66%
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“…CL int, in vivo data were provided in several reports (Shibata et al, 2002;Naritomi et al, 2003). Relationships obtained using the parallel tube model to compute CL int, in vivo were very similar to those reported (data not shown).…”
Section: Methodssupporting
confidence: 66%
“…CL int, in vitro data derived from hepatocyte (Lave et al, 1997a,b;Lau et al, 2002;Shibata et al, 2002;Naritomi et al, 2003) or microsomal incubations (Carlile et al, 1999;Obach, 1999;Naritomi et al, 2001;Andersson et al, 2004) were generated in the authors' laboratory and collated from several published studies (Tables 1-3). Incubation conditions for data generated in the authors' laboratory have been detailed previously (Austin et al, 2002;McGinnity et al, 2004).…”
Section: Methodsmentioning
confidence: 99%
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“…Gauss-Seidel iterative method with a convergence criterion of 10 -6 was used for solving the system of algebraic equations simultaneously in MATLAB. Simulation was performed for seven drugs, lidocaine, metoprolol, verapamil, caffeine, timolol, diazepam, and phenacetin (Shibata et al, 2002), at a hepatic perfusion rate of 1500 mlmin -1 and a sinusoidal porosity of 0.12 (Bonfiglio et al, 2010) for a time-course of 200 s following a 5 mg IV dose of each drug. The tortuosity of the liver tissue was calculated according to the tortuosity of porous media consisting of layer by layer parallel rods as (Perry and Green, 2008): Table 1 shows the reported pharmacokinetic properties of each drug used for the simulation.…”
mentioning
confidence: 99%