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鉴定 157 例 HPV 阳性和 HPV 阴性口咽鳞癌中的预后分子生物标志物。

Identification of prognostic molecular biomarkers in 157 HPV-positive and HPV-negative squamous cell carcinomas of the oropharynx.

机构信息

Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, NY.

Department of Surgery, Memorial Sloan Kettering Cancer Center, New York, NY.

出版信息

Int J Cancer. 2019 Dec 1;145(11):3152-3162. doi: 10.1002/ijc.32412. Epub 2019 May 30.

DOI:10.1002/ijc.32412
PMID:31093971
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7595146/
Abstract

The incidence of oropharyngeal squamous cell carcinoma (OPSCC) has been increasing due to high-risk HPV infection. We explored the significance of genetic alterations in HPV-positive (HPV-P) and HPV-negative (HPV-N) OPSCC patients on long-term outcome. A total of 157 cases of primary resected OPSCC diagnosed from 1978 to 2005 were subjected to a targeted exome sequencing by MSK-IMPACT™ interrogating somatic mutations in 410 cancer-related genes. Mutational profiles were correlated to recurrence and survival outcomes. OPSCC included 47% HPV-positive (HPV-P) and 53% HPV-negative (HPV-N) tumors arising in the base of tongue (BOT, 43%), palatine tonsil (30%) and soft palate (SP, 27%). HPV negative status, SP location and smoking were associated with poorer outcome. Poorer overall survival was found in NOTCH1-mutated HPV-P (p = 0.039), and in SOX2-amplified HPV-N cases (p = 0.036). Chromosomal arm gains in 8p and 8q, and 16q loss were more common in HPV-P (p = 0.005, 0.04 and 0.01, respectively), while 9p, 18q and 21q losses were more frequent in HPV-N OPSCC (p = 0.006, 0.002 and 0.01, respectively). Novel, potentially functional JAK3, MYC and EP300 intragenic deletions were found in HPV-P, and FOXP1, CDKN2A, CCND1 and RUNX1 intragenic deletions and one FGFR3 inversion were detected in HPV-N tumors. HPV-N/TP53-wild-type OPSCC harbored recurrent mutations in NOTCH1/3/4 (39%), PIK3CA, FAT1 and TERT. In comparison to their oral and laryngeal counterparts, HPV-N OPSCC were genetically distinct. In OPSCC, HPV status, tumor subsite and smoking determine outcome. Risk-stratification can be further refined based on the mutational signature, namely, NOTCH1 and SOX2 mutation status.

摘要

由于高危型 HPV 感染,口咽鳞状细胞癌(OPSCC)的发病率一直在上升。我们探讨了 HPV 阳性(HPV-P)和 HPV 阴性(HPV-N)OPSCC 患者中遗传改变对长期预后的意义。对 1978 年至 2005 年期间诊断的 157 例原发性切除 OPSCC 病例进行了靶向外显子组测序,该测序通过 MSK-IMPACT™对 410 个癌症相关基因中的体细胞突变进行了检测。突变谱与复发和生存结果相关。OPSCC 包括 47%的 HPV 阳性(HPV-P)和 53%的 HPV 阴性(HPV-N)肿瘤,其中舌根(BOT)占 43%,扁桃体(30%)和软腭(SP)占 27%。HPV 阴性状态、SP 位置和吸烟与较差的预后相关。NOTCH1 突变的 HPV-P(p = 0.039)和 SOX2 扩增的 HPV-N 病例(p = 0.036)的总生存率较差。HPV-P 中更常见的是 8p 和 8q 染色体臂增益以及 16q 缺失(p = 0.005、0.04 和 0.01),而 HPV-N OPSCC 中更常见的是 9p、18q 和 21q 缺失(p = 0.006、0.002 和 0.01)。在 HPV-P 中发现了潜在功能的 JAK3、MYC 和 EP300 基因内缺失,而在 HPV-N 肿瘤中发现了 FOXP1、CDKN2A、CCND1 和 RUNX1 基因内缺失和一个 FGFR3 倒位。HPV-P 中还发现了 NOV 、MYC 和 EP300 基因内缺失,HPV-N 肿瘤中还发现了 FOXP1、CDKN2A、CCND1 和 RUNX1 基因内缺失和一个 FGFR3 倒位。HPV-N/TP53 野生型 OPSCC 中存在 NOTCH1/3/4(39%)、PIK3CA、FAT1 和 TERT 的复发性突变。与口腔和喉癌相比,HPV-N OPSCC 在遗传上存在差异。在 OPSCC 中,HPV 状态、肿瘤部位和吸烟决定预后。可以根据突变特征(即 NOTCH1 和 SOX2 突变状态)进一步细化风险分层。

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