Yale Cancer Center Precision Medicine Tumor Board: new technology, new drugs, and the value of repeat testing

RET status was not evaluable due to technical failure of the assay. Since no driver alteration was detected, the patient was treated with pembrolizumab as part of a clinical trial and had prolonged disease stability. Oncogenic activation of the RET tyrosine kinase can occur via mutation of the codin...

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Bibliographic Details
Published in:The lancet oncology 2020-03, Vol.21 (3), p.343-344
Main Authors: Hafez, Navid, Walther, Zenta, Eder, Joseph P, Sklar, Jeffrey L, Gettinger, Scott N, Finberg, Karin E, Goldberg, Sarah B
Format: Article
Language:English
Subjects:
Cancer therapies
Clinical trials
Deoxyribonucleic acid
DNA
FDA approval
Gene fusion
Genes
Immunotherapy
Kinases
Laboratories
Lung cancer
Lymphatic system
Monoclonal antibodies
Mutation
Papillary thyroid cancer
Pathology
Patients
Pembrolizumab
Polymerase chain reaction
Precision medicine
Protein-tyrosine kinase
Ret protein
Ribonucleic acid
RNA
Signal transduction
Targeted cancer therapy
Thyroid cancer
Thyroid carcinoma
Tumors
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Summary:RET status was not evaluable due to technical failure of the assay. Since no driver alteration was detected, the patient was treated with pembrolizumab as part of a clinical trial and had prolonged disease stability. Oncogenic activation of the RET tyrosine kinase can occur via mutation of the coding sequence (often found in medullary thyroid carcinoma), or by chromosomal rearrangement that fuses the kinase domain of RET to a variety of partner genes (often found in papillary thyroid cancer). Others assays, such as the Oncomine assay, identify gene fusions in the tumour RNA by sequencing the products of a multiplex RT-PCR reaction designed to amplify specific fusion junctions among transcripts generated by a large set of possible gene fusions. Because oncogenic gene fusions are expected to be highly expressed, RNA-based methods might have greater sensitivity to detect gene fusion events compared with DNA-based methods in samples with low malignant cell content.
ISSN:1470-2045
1474-5488
DOI:10.1016/S1470-2045(20)30010-3