Sang Ye, Hu Guanghui, Xue Junyu, Chen Mengke, Hong Shubin, Liu Rengyun
Institute of Precision Medicine, The First Affiliated Hospital, Sun Yat-Sen University, No. 58, Zhongshan Second Road, Guangzhou, China.
Department of Endocrinology, The First Affiliated Hospital, Sun Yat-Sen University, No. 58, Zhongshan Second Road, Guangzhou, China.
Endocrine. 2024 Jul;85(1):304-312. doi: 10.1007/s12020-024-03722-6. Epub 2024 Feb 14.
Risk stratification based on somatic mutations in TERT promoter and BRAF/RAS has been well established for papillary thyroid cancer (PTC), and there is emerging evidence showed that TERT promoter methylation was frequently observed in thyroid cancer patients with adverse features. This study was aimed to comprehensive explore the prognostic value of BRAF/RAS mutations, TERT promoter mutations, and TERT promoter methylation in PTC.
The relationships of BRAF/RAS mutations, TERT promoter mutations, and TERT promoter methylation with clinical characteristics and outcomes of PTC were analyzed in 382 patients with PTC.
TERT promoter mutation and hypermethylation were collectively observed in 52 (13.6%) samples and associated with BRAF/RAS mutation, aggressive clinical characteristics, and poor clinical outcomes of PTC. Coexistence of BRAF/RAS and TERT alterations was found in 45 of 382 (11.8%) PTC patients and strongly associated with old patient age, extrathyroidal extension, advanced pathologic T stage and metastasis. Importantly, patients with both BRAF/RAS and TERT alterations had higher rates of tumor recurrence (13.6% vs 1.5%, P = 0.042) and disease progression (24.4% vs 3.3%, P < 0.001) than patients without any alterations, and cox regression analysis revealed that the coexistence of BRAF/RAS and TERT alterations, but not BRAF/RAS or TERT alterations alone, increased the risk of progression-free interval with an adjusted HR of 10.35 (95% CI: 1.79-59.81, P = 0.009).
This study suggested that comprehensively analysis of BRAF/RAS mutations, TERT promoter mutation and methylation is an effective strategy to identify high-risk patients with PTC.
基于端粒酶逆转录酶(TERT)启动子和BRAF/RAS基因的体细胞突变进行风险分层在甲状腺乳头状癌(PTC)中已得到充分确立,并且有新证据表明TERT启动子甲基化在具有不良特征的甲状腺癌患者中经常被观察到。本研究旨在全面探讨BRAF/RAS突变、TERT启动子突变和TERT启动子甲基化在PTC中的预后价值。
分析了382例PTC患者中BRAF/RAS突变、TERT启动子突变和TERT启动子甲基化与PTC临床特征及预后的关系。
在52个(13.6%)样本中共同观察到TERT启动子突变和高甲基化,且与BRAF/RAS突变、侵袭性临床特征及PTC的不良临床预后相关。在382例(11.8%)PTC患者中有45例同时存在BRAF/RAS和TERT改变,且与患者年龄较大、甲状腺外侵犯、病理T分期较高及转移密切相关。重要的是,与无任何改变的患者相比,同时存在BRAF/RAS和TERT改变的患者肿瘤复发率(13.6%对1.5%,P = 0.042)和疾病进展率(24.4%对3.3%,P < 0.001)更高,且Cox回归分析显示,BRAF/RAS和TERT改变同时存在而非单独的BRAF/RAS或TERT改变会增加无进展生存期的风险,校正后的风险比为10.35(95%可信区间:1.79 - 59.81,P = 0.009)。
本研究提示,综合分析BRAF/RAS突变、TERT启动子突变和甲基化是识别PTC高危患者的有效策略。
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