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分化型甲状腺癌原发肿瘤与配对远处转移灶中高度一致的关键基因改变

Highly Concordant Key Genetic Alterations in Primary Tumors and Matched Distant Metastases in Differentiated Thyroid Cancer.

作者信息

Sohn Seo Young, Park Woong Yang, Shin Hyun Tae, Bae Joon Seol, Ki Chang Seok, Oh Young Lyun, Kim Sun Wook, Chung Jae Hoon

机构信息

1 Department of Endocrinology and Metabolism, Seonam University , Myongji Hospital, Goyang, Korea.

2 Samsung Genome Institute, Samsung Medical Center , Seoul, Korea.

出版信息

Thyroid. 2016 May;26(5):672-82. doi: 10.1089/thy.2015.0527.

Abstract

BACKGROUND

Distant metastases uncommonly occur in differentiated thyroid carcinoma (DTC), but they are a frequent cause of thyroid cancer-related death. Genomic alterations in metastatic tumors, and the relationship with their corresponding primary tumors in DTC, are poorly understood. The objective of this study was to investigate whether genetic alterations in primary tumors are concordant with distant metastases in DTC patients.

METHODS

Surgical samples from primary and matched distant metastatic tumor pairs from 17 DTC patients, and three additional unpaired metastatic tumors from two patients, were analyzed using targeted next-generation sequencing (Ion Torrent Ampliseq cancer panel) with a focus on known recurrent somatic mutations in thyroid cancer. Additionally, TERT promoter mutations were assessed by direct sequencing.

RESULTS

BRAF mutations were found in 8/10 patients with papillary thyroid carcinoma (PTC). A NRAS mutation was detected in one patient with follicular variant PTC. TERT promoter mutations were detected in 8/10 patients with PTC, and most were coexistent with a BRAF mutation (7/8 BRAF-positive PTC patients, and one BRAF-negative PTC patient). In follicular thyroid carcinoma, NRAS was the most frequently observed mutation (4/9 patients), followed by HRAS (two patients) and KRAS (one patient). TERT promoter mutations were found in 6/7 RAS-positive follicular thyroid carcinoma patients. Key somatic alterations such as BRAF and RAS mutations were highly concordant between primary and matched metastatic tumors without discrepancies. The BRAF or RAS mutant allelic frequency was higher in matched metastatic tumors than in the corresponding primary tumors (35% vs. 25% for BRAF mutation, p = 0.04; and 40% vs. 34% for RAS mutation, p = 0.002). TERT promoter mutations were also mostly concordant in matched tumors (concordance rate 93%).

CONCLUSIONS

BRAF, RAS, and TERT mutations are highly prevalent in metastatic DTC, and are concordant between primary and metastatic DTC. This high concordance suggests that primary tumors may reflect the key somatic alterations in matched metastatic DTC. Frequent coexistent TERT promoter and BRAF or RAS mutations in metastatic DTC also suggests its important role in the progression of DTC.

摘要

背景

远处转移在分化型甲状腺癌(DTC)中并不常见,但却是甲状腺癌相关死亡的常见原因。转移性肿瘤中的基因组改变以及它们与DTC中相应原发性肿瘤的关系尚不清楚。本研究的目的是调查原发性肿瘤中的基因改变是否与DTC患者的远处转移一致。

方法

对17例DTC患者的原发性和配对远处转移肿瘤样本,以及另外2例患者的3个未配对转移肿瘤样本,使用靶向二代测序(Ion Torrent Ampliseq癌症检测板)进行分析,重点关注甲状腺癌中已知的复发性体细胞突变。此外,通过直接测序评估TERT启动子突变。

结果

在10例乳头状甲状腺癌(PTC)患者中有8例发现BRAF突变。在1例滤泡状变异型PTC患者中检测到NRAS突变。在10例PTC患者中有8例检测到TERT启动子突变,且大多数与BRAF突变共存(8例BRAF阳性PTC患者中有7例,1例BRAF阴性PTC患者)。在滤泡状甲状腺癌中,NRAS是最常观察到的突变(9例患者中有4例),其次是HRAS(2例患者)和KRAS(1例患者)。在7例RAS阳性滤泡状甲状腺癌患者中有6例发现TERT启动子突变。BRAF和RAS突变等关键体细胞改变在原发性和配对转移性肿瘤之间高度一致,没有差异。配对转移性肿瘤中BRAF或RAS突变等位基因频率高于相应原发性肿瘤(BRAF突变:35%对25%,p = 0.04;RAS突变:40%对34%,p = 0.

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