Ultrasound and clinicopathological features of papillary thyroid carcinomas with BRAF and TERT promoter mutations.

Soo Yeon Hahn,Chang Seok Ki,Tae Hyuk Kim,Jung Hee Shin,Soohyun Ahn,Jae Hoon Chung,Sun Wook Kim

doi:10.18632/oncotarget.22430

Abstract

This study is to investigate if any relationship exists between the telomerase reverse transcriptase (TERT) promoter or proto-oncogene BRAF mutation and ultrasound (US) and clinicopathological features of papillary thyroid carcinomas (PTCs). The study included 150 patients with surgically confirmed PTC from October 1994 to December 2004. According to the existence of TERT promoter or BRAF mutations, we categorized patients into three groups (no mutation, BRAF mutation alone, or TERT+BRAF mutations) and analyzed the relationships between TERT promoter or BRAF mutation and US and clinicopathological features. The rate of recurrence or death according to mutation analysis was estimated. There were 35 (23.3%) cases with no mutation, 104 (69.3%) with BRAF mutation alone, and 11 (7.3%) with TERT+BRAF mutations. As the number of genetic mutations increased from no mutation to BRAF mutation alone to both BRAF and TERT mutations, the proportions of hypoechogenicity, non-parallel orientation, spiculated/microlobulated margin, microcalcifications, and high suspicion category increased. PTCs with TERT+BRAF mutations recurred more frequently than other groups (odd ratio = 17.921 and 31.468). The intervals to recurrence and overall survival were significantly shorter in the TERT+BRAF mutation group than in the other groups (Ps <.0001). PTCs with no mutation, with BRAF mutation alone, and with both TERT and BRAF mutations linearly increase in the probability of displaying malignant US features. In PTCs, the coexistence of BRAF with TERT mutations is more strongly correlated with recurrence and mortality than BRAF mutation alone.

Highlights

Papillary thyroid carcinoma (PTC) is the most common type of thyroid cancer, accounting for 70–90%of well-differentiated thyroid malignancies [1]
The BRAF mutation was found in 69.3% (104 of 150) of PTCs, whereas the telomerase reverse transcriptase (TERT) promoter mutation was found in 7.3% (11 of 150) of PTCs
Extrathyroidal extension of PTC, surgical margin involvement, lateral lymph node metastasis, advanced TNM stage, recurrence, and death were more common in the TERT+BRAF mutation group than in the BRAF mutation alone group (P =.0052, P =.0089, P = 0.0002, P =.0007, P

Summary

Introduction

Papillary thyroid carcinoma (PTC) is the most common type of thyroid cancer, accounting for 70–90%of well-differentiated thyroid malignancies [1]. PTC generally displays an indolent clinical course and has excellent prognosis despite 15–30% local or regional recurrence [2,3,4]. Some PTCs exhibit www.impactjournals.com/oncotarget more aggressive characteristics and may cause mortality. Various risk stratification methods have been used for the appropriate management of patients with thyroid cancer; none are completely accurate. Molecular biomarkers have been investigated as adjunct diagnostic markers of thyroid cancer and as predictors of patient prognosis. The prognostic impact of BRAF mutations in patient mortality remains controversial [10, 11]. Additional prognostic biomarkers to predict aggressive disease are needed

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