Evaluation of crizotinib absolute bioavailability, the bioequivalence of three oral formulations, and the effect of food on crizotinib pharmacokinetics in healthy subjects

Xu, Huiping; O'Gorman, Melissa; Boutros, Tanya; Brega, Nicoletta; Kantaridis, Constantino; Tan, Weiwei; Bello, Akintunde

doi:10.1002/jcph.356

Cited by 39 publications

(36 citation statements)

References 12 publications

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“…In the single-dose oral bioavailability study, crizotinib oral bioavailability was estimated to be 0.43 with an F a Â F g value of 0.96 in healthy subjects at an oral dose of 250 mg relative to an intravenous dose of 50 mg, assuming linear pharmacokinetics (Xu et al, 2015). Using the model-predicted F g value of 0.94, F a was calculated to be ;0.9 in this study.…”

Section: Discussionmentioning

confidence: 93%

“…Crizotinib hepatic microsomal intrinsic clearance (CL int,hep ) was back-calculated from the clinically observed plasma clearance (CL) using a retrograde model implemented in Simcyp version 13.1 (Jamei et al, 2009). Crizotinib intravenous and oral plasma CL estimates (geometric mean) were 46.8 and 108 l/h, respectively, in the single-dose oral bioavailability study (Xu et al, 2015). In the crizotinib single-dose DDI studies with ketoconazole and rifampin, crizotinib oral plasma CL estimates in the control groups (crizotinib alone) were 123 and 119 l/h, respectively (Xu et al, 2011a(Xu et al, , 2011b.…”

Section: Methodsmentioning

confidence: 99%

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Prediction of Drug-Drug Interactions with Crizotinib as the CYP3A Substrate Using a Physiologically Based Pharmacokinetic Model

2015

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An orally available multiple tyrosine kinase inhibitor, crizotinib (Xalkori), is a CYP3A substrate, moderate time-dependent inhibitor, and weak inducer. The main objectives of the present study were to: 1) develop and refine a physiologically based pharmacokinetic (PBPK) model of crizotinib on the basis of clinical single-and multiple-dose results, 2) verify the crizotinib PBPK model from crizotinib single-dose drug-drug interaction (DDI) results with multiple-dose coadministration of ketoconazole or rifampin, and 3) apply the crizotinib PBPK model to predict crizotinib multiple-dose DDI outcomes. We also focused on gaining insights into the underlying mechanisms mediating crizotinib DDIs using a dynamic PBPK model, the Simcyp population-based simulator. First, PBPK model-predicted crizotinib exposures adequately matched clinically observed results in the single-and multiple-dose studies. Second, the model-predicted crizotinib exposures sufficiently matched clinically observed results in the crizotinib single-dose DDI studies with ketoconazole or rifampin, resulting in the reasonably predicted fold-increases in crizotinib exposures. Finally, the predicted fold-increases in crizotinib exposures in the multipledose DDI studies were roughly comparable to those in the singledose DDI studies, suggesting that the effects of crizotinib CYP3A time-dependent inhibition (net inhibition) on the multiple-dose DDI outcomes would be negligible. Therefore, crizotinib doseadjustment in the multiple-dose DDI studies could be made on the basis of currently available single-dose results. Overall, we believe that the crizotinib PBPK model developed, refined, and verified in the present study would adequately predict crizotinib oral exposures in other clinical studies, such as DDIs with weak/ moderate CYP3A inhibitors/inducers and drug-disease interactions in patients with hepatic or renal impairment.

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Section: Discussionmentioning

confidence: 93%

Section: Methodsmentioning

confidence: 99%

Prediction of Drug-Drug Interactions with Crizotinib as the CYP3A Substrate Using a Physiologically Based Pharmacokinetic Model

2015

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“…The pharmacokinetics of crizotinib in adults has been studied after a single dose and at steady state (≥15 days) in patients with NSCLC using 250-mg formulated capsules and after a single 50-mg dose of an experimental intravenous formulation or a single 250-mg dose of three oral formulations [formulated capsules (FC), powder in capsules (PIC) and immediate-release tablets (IRT)] in healthy volunteers [8, 9]. The mean (C.V.) clearance (CL) of crizotinib was 47 (18%) L/h, the volume of distribution at steady state was 1770 (18%) L and the half-life ( T 1/2 ) was 39 (16%) h, following the intravenous dose.…”

Section: Introductionmentioning

confidence: 99%

First-dose and steady-state pharmacokinetics of orally administered crizotinib in children with solid tumors: a report on ADVL0912 from the Children’s Oncology Group Phase 1/Pilot Consortium

Balis

Thompson

Mossé

et al. 2016

Cancer Chemother Pharmacol

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Purpose Characterize the pharmacokinetics of oral crizotinib in children with cancer.MethodsSixty-four children with solid tumors or anaplastic large-cell lymphoma (ALCL) enrolled on a phase 1/2 trial of the ALK, MET and ROS1 inhibitor, crizotinib, had pharmacokinetic sampling after the first dose (n = 15) or at steady state (n = 49). Dose levels studied were 100, 130, 165, 215, 280 and 365 mg/m2/dose administered twice daily. Two capsule and two oral liquid formulations were used over the course of the trial. Crizotinib was quantified with a validated HPLC/tandem mass spectrometry method with a lower limit of detection of 0.2 ng/mL. Pharmacokinetic parameters were derived using non-compartmental analysis.ResultsTime to peak plasma concentration was 4 h. At 280 mg/m2 (MTD), mean (±SD) steady-state peak plasma concentration was 717 ± 201 ng/mL, and steady-state trough plasma concentration was 480 ± 176 ng/mL. At steady state, AUC0–τ was proportional to dose over the dose range of 215–365 mg/m2/dose. Apparent clearance of crizotinib was 731 ± 241 mL/min/m2. Steady-state AUC0–τ at 280 mg/m2/dose was 2.5-fold higher than the AUC0–∞ in adults receiving 250 mg (~140 mg/m2). Age, sex and drug formulation do not account for the inter-subject variability in AUC0–τ at steady state. The accumulation index was 4.9, and the half-life estimated from the accumulation index was 36 h.ConclusionsThe pharmacokinetics of oral crizotinib in children is similar to that in adults. Steady-state trough-free crizotinib concentrations in plasma at the MTD exceed inhibitory concentrations of crizotinib in ALCL cell lines.ClinicalTrials.gov identifierNCT00939770.

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“…administration and 250 mg oral administration with the assumption that hepatic clearance was identical. [23] No data has been reported on the bioavailability of ceritinib. Although the specific cytochrome-P (CYP) enzymes for ceritinib are unknown, both drugs are metabolized by CYP3A enzymes, with crizotinib primarily by CYP3A4/5.…”

Section: Pharmacokineticsmentioning

confidence: 99%

“…If we assume these numbers are correct, at least twice as much ceritinib is needed to reach the *Calculated by comparing I.V. and oral administration with the assumption that hepatic clearance was identical [23] optimal concentration in plasma, considering ceritinib has a V d twice as large as crizotinib. However, ceritinib is 6 times more potent in inhibiting the growth of Ba/F3 ALK-positive cell lines than crizotinib, implying that a 6-fold lower concentration is as effective in vitro in ALKinhibition as crizotinib.…”

Section: Pharmacokineticsmentioning

confidence: 99%

Overcoming crizotinib resistance in ALK-rearranged NSCLC with the second-generation ALK-inhibitor ceritinib

Muller

Langen

Honeywell

et al. 2016

Expert Review of Anticancer Therapy

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In up to 5% of non-small cell lung cancer (NSCLC) patients, the EML4-ALK translocation drives tumor progression. Treatment with the ALK inhibitor crizotinib is more effective than standard chemotherapy. However, resistance to crizotinib occurs after approximately 8 months. Ceritinib is the first second-generation ALK inhibitor approved for treatment of crizotinib-resistant NSCLC. Ceritinib inhibits two of the most common ALK-mutants that confer resistance to crizotinib: L1196 M and G1269A. Cells with ALK expression are more sensitive to ceritinib than crizotinib (IC 50 25 nM vs. 150 nM, respectively). Alternative second-generation ALK inhibitors such as Alectinib, Brigatinib and PF-06463922 are currently in development, each affecting different crizotinib-resistant ALK target mutations. Genetic identification of crizotinib-resistant mutants is essential for selecting the optimal treatment strategy in NSCLC patients to overcome resistance and to increase progression-free survival.ARTICLE HISTORY

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Evaluation of crizotinib absolute bioavailability, the bioequivalence of three oral formulations, and the effect of food on crizotinib pharmacokinetics in healthy subjects

Cited by 39 publications

References 12 publications

Prediction of Drug-Drug Interactions with Crizotinib as the CYP3A Substrate Using a Physiologically Based Pharmacokinetic Model

Prediction of Drug-Drug Interactions with Crizotinib as the CYP3A Substrate Using a Physiologically Based Pharmacokinetic Model

First-dose and steady-state pharmacokinetics of orally administered crizotinib in children with solid tumors: a report on ADVL0912 from the Children’s Oncology Group Phase 1/Pilot Consortium

Overcoming crizotinib resistance in ALK-rearranged NSCLC with the second-generation ALK-inhibitor ceritinib

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