Genetic Alterations and Their Clinical Implications in High-Recurrence Risk Papillary Thyroid Cancer.

Min Young Lee; Bo Mi KU; Hae Su Kim; Ji Yun Lee; Sung Hee Lim; Jong Mu Sun; Se Hoon Lee; Keunchil Park; Young Lyun OH; Mineui Hong; Han Sin Jeong; Young Ik Son; Chung Hwan Baek; Myung Ju Ahn

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Genetic Alterations and Their Clinical Implications in High-Recurrence Risk Papillary Thyroid Cancer.

Author: Min Young LEE ¹ ; Bo Mi KU ; Hae Su KIM ; Ji Yun LEE ; Sung Hee LIM ; Jong Mu SUN ; Se Hoon LEE ; Keunchil PARK ; Young Lyun OH ; Mineui HONG ; Han Sin JEONG ; Young Ik SON ; Chung Hwan BAEK ; Myung Ju AHN
Author Information

1. Division of Hematology-Oncology, Department of Medicine, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea. silkahn@skku.edu
Publication Type:Original Article
Keywords: Papillary thyroid carcinoma; BRAF; PIK3CA; RET
MeSH: Gene Fusion; Humans; Retrospective Studies; Sequence Analysis, DNA; Thyroid Gland*; Thyroid Neoplasms*
From:Cancer Research and Treatment 2017;49(4):906-914
CountryRepublic of Korea
Language:English
Abstract: PURPOSE: Papillary thyroid carcinomas (PTCs) frequently involve genetic alterations. The objective of this study was to investigate genetic alterations and further explore the relationships between these genetic alterations and clinicopathological characteristics in a high-recurrence risk (node positive, N1) PTC group. MATERIALS AND METHODS: Tumor tissue blocks were obtained from 240 surgically resected patients with histologically confirmed stage III/IV (pT3/4 or N1) PTCs. We screened gene fusions using NanoString’s nCounter technology and mutational analysis was performed by direct DNA sequencing. Data describing the clinicopathological characteristics and clinical courses were retrospectively collected. RESULTS: Of the 240 PTC patients, 207 (86.3%) had at least one genetic alteration, including BRAF mutation in 190 patients (79.2%), PIK3CA mutation in 25 patients (10.4%), NTRK1/3 fusion in six patients (2.5%), and RET fusion in 24 patients (10.0%). Concomitant presence of more than two genetic alterations was seen in 36 patients (15%). PTCs harboring BRAF mutation were associated with RET wild-type expression (p=0.001). RET fusion genes have been found to occur with significantly higher frequency in N1b stage patients (p=0.003) or groups of patients aged 45 years or older (p=0.031); however, no significant correlation was found between other genetic alterations. There was no trend toward favorable recurrence-free survival or overall survival among patients lacking genetic alterations. CONCLUSION: In the selected high-recurrence risk PTC group, most patients had more than one genetic alteration. However, these known alterations could not entirely account for clinicopathological features of high-recurrence risk PTC.