Evaluation of the drug–drug interaction potential of brigatinib using a physiologically‐based pharmacokinetic modeling approach

Michael J. Hanley; Karen Rowland Yeo; Meera Tugnait; Shinji Iwasaki; Narayana Narasimhan; Pingkuan Zhang; Karthik Venkatakrishnan; Neeraj Gupta

doi:10.1002/psp4.13106

CPT: Pharmacometrics & Systems Pharmacology (Apr 2024)

Evaluation of the drug–drug interaction potential of brigatinib using a physiologically‐based pharmacokinetic modeling approach

Michael J. Hanley,
Karen Rowland Yeo,
Meera Tugnait,
Shinji Iwasaki,
Narayana Narasimhan,
Pingkuan Zhang,
Karthik Venkatakrishnan,
Neeraj Gupta

Affiliations

Michael J. Hanley: Clinical Pharmacology, Takeda Development Center Americas, Inc. Lexington Massachusetts USA
Karen Rowland Yeo: Simcyp Division, Certara UK Limited Sheffield, South Yorkshire UK
Meera Tugnait: Clinical Pharmacology, Cerevel Therapeutics Cambridge Massachusetts USA
Shinji Iwasaki: Global DMPK, Takeda Development Center Americas, Inc. Lexington Massachusetts USA
Narayana Narasimhan: DMPK & Preclinical Safety, Theseus Pharmaceuticals Cambridge Massachusetts USA
Pingkuan Zhang: Clinical Science, Takeda Development Center Americas, Inc. Lexington Massachusetts USA
Karthik Venkatakrishnan: Quantitative Pharmacology, EMD Serono Research & Development Institute, Inc. Billerica Massachusetts USA
Neeraj Gupta: Clinical Pharmacology, Takeda Development Center Americas, Inc. Lexington Massachusetts USA

DOI: https://doi.org/10.1002/psp4.13106
Journal volume & issue: Vol. 13, no. 4
pp. 624 – 637

Abstract

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Abstract Brigatinib is an oral anaplastic lymphoma kinase (ALK) inhibitor approved for the treatment of ALK‐positive metastatic non‐small cell lung cancer. In vitro studies indicated that brigatinib is primarily metabolized by CYP2C8 and CYP3A4 and inhibits P‐gp, BCRP, OCT1, MATE1, and MATE2K. Clinical drug–drug interaction (DDI) studies with the strong CYP3A inhibitor itraconazole or the strong CYP3A inducer rifampin demonstrated that CYP3A‐mediated metabolism was the primary contributor to overall brigatinib clearance in humans. A physiologically‐based pharmacokinetic (PBPK) model for brigatinib was developed to predict potential DDIs, including the effect of moderate CYP3A inhibitors or inducers on brigatinib pharmacokinetics (PK) and the effect of brigatinib on the PK of transporter substrates. The developed model was able to predict clinical DDIs with itraconazole (area under the plasma concentration–time curve from time 0 to infinity [AUC∞] ratio [with/without itraconazole]: predicted 1.86; observed 2.01) and rifampin (AUC∞ ratio [with/without rifampin]: predicted 0.16; observed 0.20). Simulations using the developed model predicted that moderate CYP3A inhibitors (e.g., verapamil and diltiazem) may increase brigatinib AUC∞ by ~40%, whereas moderate CYP3A inducers (e.g., efavirenz) may decrease brigatinib AUC∞ by ~50%. Simulations of potential transporter‐mediated DDIs predicted that brigatinib may increase systemic exposures (AUC∞) of P‐gp substrates (e.g., digoxin and dabigatran) by 15%–43% and MATE1 substrates (e.g., metformin) by up to 29%; however, negligible effects were predicted on BCRP‐mediated efflux and OCT1‐mediated uptake. The PBPK analysis results informed dosing recommendations for patients receiving moderate CYP3A inhibitors (40% brigatinib dose reduction) or inducers (up to 100% increase in brigatinib dose) during treatment, as reflected in the brigatinib prescribing information.

Published in CPT: Pharmacometrics & Systems Pharmacology

ISSN: 2163-8306 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: https://ascpt.onlinelibrary.wiley.com/journal/21638306

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