Abstract
BackgroundMutations in the telomerase reverse transcriptase (TERT) promoter region have been proposed as novel mechanisms for the transcriptional activation of telomerase. Two recurrent mutations in the TERT promoter, C228T and C250T, are prognostic biomarkers. Herein, we directly compared the commercially available iTERT PCR kit with NGS-based deep sequencing to validate the NGS results and determine the analytical sensitivity of the PCR kit.MethodsOf the 2032 advanced solid tumors diagnosed using the TruSight Oncology 500 NGS test, mutations in the TERT promoter region were detected in 103 cases, with 79 cases of C228T, 22 cases of C250T, and 2 cases of C228A hotspot mutations. TERT promoter mutations were detected from 31 urinary bladder, 19 pancreato-biliary, 22 hepatic, 12 malignant melanoma, and 12 other tumor samples.ResultsIn all 103 TERT-mutated cases detected using NGS, the same DNA samples were also tested with the iTERT PCR/Sanger sequencing. PCR successfully verified the presence of the same mutations in all cases with 100% agreement. The average read depth of the TERT promoter region was 320.4, which was significantly lower than that of the other genes (mean, 743.5). Interestingly, NGS read depth was significantly higher at C250 compared to C228 (p < 0.001).ConclusionsThe NGS test results were validated by a PCR test and iTERT PCR/Sanger sequencing is sensitive for the identification of the TERT promoter mutations.
Highlights
Mutations in the telomerase reverse transcriptase (TERT) promoter region have been proposed as novel mechanisms for the transcriptional activation of telomerase
Patients samples In this study, we used a total of 103 cases diagnosed with TERT promoter mutations at the C228T and C250T hotspots using the TruSight Oncology (TSO) 500 next-generation sequencing (NGS) test in the Department of Pathology and Translation Genomics of Samsung Medical Center between November 2019 and March 2021
NGS with TSO 500 TERT promoter mutations were detected in 103 (5.1%) out of 2032 cases and consisted of 79 (77%) C228T, 22 (21%) C250T, and 2 (2%) C228A mutations. Of these 103 cases, the TERT promoter mutations were detected in urinary bladder tumor (31/47, 66%), pancreato-biliary (19/127, 15%), hepatocellular carcinoma (22/41, 54%), and malignant melanoma (12/90, 13%)
Summary
Mutations in the telomerase reverse transcriptase (TERT) promoter region have been proposed as novel mechanisms for the transcriptional activation of telomerase. Two recurrent mutations in the TERT promoter, C228T and C250T, are prognostic biomarkers. Mutations in the telomerase reverse transcriptase (TERT) promoter region are frequently observed in specific types of human cancers, leading to enhanced expression of telomerase. Transcriptional activation of TERT via mutation in the promoter region or other mechanisms limits the production of active telomerase in many human cancers [8]. The prognostic power of the TERT promoter mutation highlights its potential use as an important biomarker to predict the aggressive clinical behavior in melanoma, glioma, medulloblastoma, bladder cancer, thyroid cancer, urogenital cancer, and laryngeal cancer [9,10,11]. TERT promoter mutation is associated with worse prognosis in melanoma, glioma, meningioma, thyroid cancer, and bladder cancer [12,13,14,15,16,17,18] and is associated with a high risk of malignant transformation and progression to advanced stages in hepatocellular carcinoma [19, 20]
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