Abstract 2222P
Background
TERT (Chr.5p15) is one of the most relevant biomarkers in thyroid cancer aggressiveness, including metastatic papillary thyroid carcinomas (mPTCs). The TERT promoter mutations (TPM) rate in mPTCs is 45-60%. Chromosomal gains at 5p have also been reported in thyroid cancer, however little is known about the specific prevalence of TERT copy number variations (CNV) in mPTCs and its putative role in tumor prognosis.
Methods
By genotyping 38 cases of primary PTCs and matched distant (DM) and/or lymphatic metastases (LNM), we sought to determine the prevalence of TPM and CNV, their coexistence, and their association with other driver mutational events in thyroid cancers. 114 areas were analyzed to tackle the contribution of intratumoral heterogeneity (ITGH) and clonal evolution to metastases. Mutational analysis was approached through PCR-SSCP or direct sequencing. Ligation-dependent probe amplification was used to assess TERT CNV.
Results
TERT was altered in 37 cases. Gains were more common than TPM (94,6% vs 45,9%). Both features coexisted in 40,5% of the cases. The study of ITGH evidenced that 66,6% and 20% of the cases bearing both, TPM + CNV, were concurrently mutated at BRAF and RAS respectively. The coexistence of both events or TPM alone correlated significantly with the stage at diagnosis (dx) and stage at follow-up (Fup), patient status (DOD, AWD, NED), age ≥ 55, and sex or showed a trend of correlation with LNM at Fup. TPM were as well significantly associated with LNM at dx and tumor recurrences, revealing a trend for an association with vascular invasion, DM, and DM at Fup too. CNV were more frequently clonal than TPM (85,7% vs 52,9%).
Conclusions
The prevalence of TERT gains in mPTCs is strikingly higher than in other cohorts of nonaggressive PTCs, such as TCGA. TERT gains tend to be more clonal than TPM. TERT CNVs seemingly represent an earlier event than TPM in mPTC. The coexistence of both events strengthens the association of TPM with poor prognostic features and tumor aggressiveness.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
Valladolid University.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
2347P - Correlation between second primary cancers and first primary cancers: A systematic review and meta-analysis of 9 million cancer patients
Presenter: Xinyu Wang
Session: Poster session 16
2348P - High-throughput screening reveals GSK1838705A as a potent inhibitor of CAFs-promoted tumor progression in esophageal squamous cell carcinoma
Presenter: hongfang zhang
Session: Poster session 16
2349P - Patterns and frequency of pathogenic germline variants (PGVs) among non-western young male patients with cancer: The Jordanian exploratory cancer genetics (Jo-ECAG) study
Presenter: Hira Bani Hani
Session: Poster session 16
2350P - Single-cell RNA-seq dissecting the initiating liver metastasis cells in various cancers
Presenter: Shu-yue Zheng
Session: Poster session 16
2351P - Whole genome sequencing of AYA patients
Presenter: Paul Roepman
Session: Poster session 16
2352P - Sex-based differences in genomic alterations and biomarkers in anal squamous cell carcinoma (ASCC)
Presenter: Stefano Cereda
Session: Poster session 16
2353P - Anti-cancer effects of HDAC8 specific inhibitors EC-352H and EC-374H in lymphoma
Presenter: So Young Lee
Session: Poster session 16
2354P - Computational pathology-derived features capture varied epithelial-mesenchymal transition (EMT) states
Presenter: Herbert Levine
Session: Poster session 16
2355P - Carcinoembryonic antigen (CEA) expression in human tumors: A tissue microarray study on 15,413 tumors
Presenter: Kristina Jansen
Session: Poster session 16
2356P - The role of pathological features in predicting prognosis of patients with advanced RET-positive NSCLC
Presenter: Arianna Marinello
Session: Poster session 16