KRAS G12V Mutation in Acquired Resistance to Combined BRAF and MEK Inhibition in Papillary Thyroid Cancer

Author:

Owen Dwight H.1,Konda Bhavana1,Sipos Jennifer2,Liu Tom3,Webb Amy4,Ringel Matthew D.2,Timmers Cynthia D.35,Shah Manisha H.1

Affiliation:

1. aDivision of Medical Oncology,

2. bDivision of Endocrinology, Diabetes, and Metabolism,

3. cSolid Tumor Translational Service, and

4. dDepartment of Biomedical Information, The Ohio State University Wexner Medical Center and Comprehensive Cancer Center, Columbus, Ohio; and

5. eMedical University of South Carolina, Charleston, South Carolina.

Abstract

BRAFV600E mutations occur in approximately 40% of all patients with papillary thyroid cancer (PTC) and are associated with a worse prognosis in population studies. Treatment with single-agent BRAF inhibitors can result in nondurable partial responses (PRs) in clinical trials, but resistance inevitably develops. The mechanisms of resistance are not completely understood, but in non-thyroid tumors harboringBRAFV600E mutations, resistance has been ascribed to concurrent or acquired mutations inMEK1/2, RAC1, KRAS,andNRAS.This case report describes a patient with radioactive iodine–refractory metastatic PTC treated in a clinical trial with combination BRAF and MEK inhibition who achieved a durable PR. At time of progression, biopsy revealed an acquiredKRASG12V–activating mutation. The patient subsequently went on to have a PR to cabozantinib therapy in the clinical trial. This is the first reported case of an acquiredKRAS-activating mutation that developed during treatment with BRAF and MEK inhibition in a patient withBRAF-mutated PTC. TheKRASmutation was also detected in peripheral blood samples taken as part of the trial, indicating that resistant mutations may be identified through noninvasive means. The identification of resistant mutations in patients at time of progression is necessary to identify possible therapeutic options including potential clinical trials.ClinicalTrials.govidentifier: NCT01723202

Publisher

Harborside Press, LLC

Subject

Oncology

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