Prediction of Oral Pharmacokinetics of cMet Kinase Inhibitors in Humans: Physiologically Based Pharmacokinetic Model Versus Traditional One-Compartment Model

Yamazaki, Shinji; Skaptason, Judith; Romero, David; Vekich, Sylvia; Jones, Hannah M.; Tan, Weiwei; Wilner, Keith D.; Koudriakova, Tatiana

doi:10.1124/dmd.110.035857

Cited by 59 publications

(49 citation statements)

References 35 publications

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“…Yamazaki et al (2011) demonstrated that a PBPK model provided better prediction of the maximum plasma concentration and the area under the plasma concentration-time curves for two compounds than a traditional one-compartment model based on CL and V ss predicted by allometric scaling. Comparative analysis between the Dedrick and PBPK approaches was conducted by Jones et al (2006), who employed 19 compounds with a wide range of CL and V ss .…”

Section: Discussionmentioning

confidence: 99%

Application of Hybrid Approach Based on Empirical and Physiological Concept for Predicting Pharmacokinetics in Humans—Usefulness of Exponent on Prospective Evaluation of Predictability

2012

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We developed a hybrid method for predicting plasma concentration-time curves in humans by integrating species differences in in vitro intrinsic clearance (CL int ) into the Dedrick approach based on the allometry concept. With prediction of clearance (CL) by allometric scaling, taking in vitro CL int into consideration improved the accuracy and reduced the average fold error from 2.72 to 1.99. With the hybrid approach of applying the same concept to the Dedrick approach, the predictability of plasma concentration profiles was compared with the results of the conventional Dedrick approach and the physiologically based pharmacokinetic model using 15 compounds with widely ranging physicochemical and pharmacokinetic profiles. The hybrid approach showed the highest predictability among the examined methods. For CL and the apparent volume of distribution at the steady state (V ss ), the relationship between the exponent of allometric equation and fold error was also evaluated with the hybrid approach. The relationship appeared to be a horseshoe curve. Six compounds with exponents ranging from 0.7 to 1.1 for both CL and V ss [antipyrine, caffeine, epiroprim, propafenone, theophylline, and verapamil] displayed higher predictability. Three compounds with an exponent ranging from 0.7 to 1.1 for CL showed better predictability for CL, and the other four compounds appeared to display similar relationship between the exponent and predictability for V ss . These findings indicated that the exponent becomes a preliminary index to speculate on predictability. Combination of the hybrid approach and exponent allows us to prospectively draw human plasma concentration-time curves, with the implication of possible prediction accuracy prior to clinical studies.

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Section: Discussionmentioning

confidence: 99%

Application of Hybrid Approach Based on Empirical and Physiological Concept for Predicting Pharmacokinetics in Humans—Usefulness of Exponent on Prospective Evaluation of Predictability

2012

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“…In GTL16 GC xenograft models, crizotinib-mediated MET inhibition was achieved with an in vivo EC 50 of 1.5 nM free, that was approximately 7-fold lower than in vitro value (10 nM) (46). While there are several potential reasons for such a disconnect between in vitro and in vivo EC 50 estimates, a correction for non-specific binding of crizotinib in the in vitro cell-based assay might be the one to be considered since crizotinib showed relatively high non-specific binding (∼90%) in hepatic microsomes and hepatocytes, along with high plasma protein binding of 91 to 96% across species (47). Another potential contributing factor could be the impact of subcutaneous inoculation of tumor cells on the expression levels of drug-metabolizing enzymes and transporters in mouse xenograft models (48), since crizotinib has been characterized as a substrate of CYP3A isozymes and multidrug-resistance transport protein, P-glycoprotein (44).…”

Section: Building Pkpd Understanding In Nonclinical Modelsmentioning

confidence: 99%

“…Crizotinib consistently showed a relatively large V ss (13 to 25 L/kg) across species including humans after an intravenous administration, and crizotinib C max was occurred at relatively later time point (e.g., 4 to 6 h) after an oral administration across species (44,47). Crizotinib has an extensive tumor distribution profiles with an approximate tumor/plasma AUC ratio of 4 at steady-state (in-house data).…”

Section: Building Pkpd Understanding In Nonclinical Modelsmentioning

confidence: 99%

Translational Pharmacokinetic-Pharmacodynamic Modeling from Nonclinical to Clinical Development: A Case Study of Anticancer Drug, Crizotinib

Yamazaki

2012

AAPS J

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Abstract. Attrition risk related to efficacy is still a major reason why new chemical entities fail in clinical trials despite recently increased understanding of translational pharmacology. Pharmacokinetic-pharmacodynamic (PKPD) analysis is key to translating in vivo drug potency from nonclinical models to patients by providing a quantitative assessment of in vivo drug potency with mechanistic insight of drug action. The pharmaceutical industry is clearly moving toward more mechanistic and quantitative PKPD modeling to have a deeper understanding of translational pharmacology. This paper summarizes an anticancer drug case study describing the translational PKPD modeling of crizotinib, an orally available, potent small molecule inhibitor of multiple tyrosine kinases including anaplastic lymphoma kinase (ALK) and mesenchymal-epithelial transition factor (MET), from nonclinical to clinical development. Overall, the PKPD relationships among crizotinib systemic exposure, ALK or MET inhibition, and tumor growth inhibition (TGI) in human tumor xenograft models were well characterized in a quantitative manner using mathematical modeling: the results suggest that 50% ALK inhibition is required for >50% TGI whereas >90% MET inhibition is required for >50% TGI. Furthermore, >75% ALK inhibition and >95% MET inhibition in patient tumors were projected by PKPD modeling during the clinically recommended dosing regimen, twice daily doses of crizotinib 250 mg (500 mg/day). These simulation results of crizotinib-mediated ALK and MET inhibition appeared consistent with the currently reported clinical responses. In summary, the present paper presents an anticancer drug example to demonstrate that quantitative PKPD modeling can be used for predictive translational pharmacology from nonclinical to clinical development.

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“…Reports of a phase II trial with AMG 102 identified that although the drug brought about tumour burden reduction and long-term disease stability, it was unclear from the study whether this drug is capable of tumour growth inhibition in a histologically diverse population of patients with mRCC (Schoffski et al, 2010). Other drugs currently in development include foretinib (GSK1363089) an oral multi kinase inhibitor of MET and VEGFRs (Kataoka et al, 2011) (Yamazaki et al, 2011). The efficacy of these drugs have yet to be investigated in patients with RCC.…”

Section: Hgf/met Signallingmentioning

confidence: 99%

Exploitation of Aberrant Signalling Pathways as Useful Targets for Renal Clear Cell Carcinoma Therapy

O’Callaghan¹,

Barry²

2011

Renal Cell Carcinoma

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Prediction of Oral Pharmacokinetics of cMet Kinase Inhibitors in Humans: Physiologically Based Pharmacokinetic Model Versus Traditional One-Compartment Model

Cited by 59 publications

References 35 publications

Application of Hybrid Approach Based on Empirical and Physiological Concept for Predicting Pharmacokinetics in Humans—Usefulness of Exponent on Prospective Evaluation of Predictability

Application of Hybrid Approach Based on Empirical and Physiological Concept for Predicting Pharmacokinetics in Humans—Usefulness of Exponent on Prospective Evaluation of Predictability

Translational Pharmacokinetic-Pharmacodynamic Modeling from Nonclinical to Clinical Development: A Case Study of Anticancer Drug, Crizotinib

Exploitation of Aberrant Signalling Pathways as Useful Targets for Renal Clear Cell Carcinoma Therapy

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