AI Article Synopsis

  • A study evaluated clinical and molecular outcomes in differentiated thyroid carcinoma (DTC) across three groups: small tumors (≤ 40 mm), large tumors (> 40 mm), and those with distant metastases.
  • Patients with metastatic DTC had the worst outcomes, experiencing higher rates of persistent disease, death, and need for further treatment, while outcomes were similar for non-metastatic groups regardless of size.
  • Genetic analysis revealed distinct mutation patterns, with TERT promoter mutations indicating a worse prognosis, particularly in metastatic cases, and BRAF mutations being more common in smaller tumors.

Article Abstract

Only a minority of cases of differentiated thyroid carcinoma (DTC) have a poor clinical outcome. Clinical outcomes and molecular aspects were assessed in: 144 DTC ≤ 40 mm without distant metastases (group 1); 50 DTC > 40 mm without distant metastases (group 2); and 46 DTC with distant metastases (group 3). Group 3 had a worse outcome than the other two groups: during the follow-up, patients more frequently had persistent disease, died, or underwent further treatment. The outcomes did not differ between groups 1 and 2. Group 3 had a higher prevalence of TERT promoter mutations than group 2 (32.6% vs 14%). Group 1 had a higher frequency of BRAF mutations than groups 2 or 3 (61.1% vs 16.0% and 26.1%, respectively), while RAS mutations were more common in group 2 than in groups 1 and 3 (16.0% vs 2.1% and 6.5%, respectively). Groups 1 and 2 shared the same outcome, but were genetically distinct. Only lymph node involvement, distant metastases, older age and (among the molecular markers) TERT promoter mutations were independent predictors of a worse outcome. Metastatic DTC had the worst outcome, while the outcome was identical for large and small non-metastatic DTC, although they showed different molecular patterns. TERT promoter mutations emerged as an independent factor pointing to a poor prognosis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8012699PMC
http://dx.doi.org/10.1038/s41598-021-86611-6DOI Listing

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