根据世界卫生组织2015年标准重新分类的一组肺大细胞癌的下一代测序
Next-Generation Sequencing of a Cohort of Pulmonary Large Cell Carcinomas Reclassified by World Health Organization 2015 Criteria.
作者信息
Driver Brandon R, Portier Bryce P, Mody Dina R, Deavers Michael, Bernicker Eric H, Kim Min P, Teh Bin S, Santacruz Jose F, Kopas Lisa, Munden Reginald F, Cagle Philip T
机构信息
From the Departments of Pathology and Genomic Medicine (Drs Driver, Portier, Mody, Deavers, and Cagle); Medicine, Thoracic Medical Oncology (Dr Bernicker); Thoracic Surgery (Dr Kim); Radiation Oncology (Dr Teh); Interventional Pulmonology, Critical Care, and Pulmonary Medicine (Drs Santacruz and Kopas); Radiology (Dr Munden), Houston Methodist Hospital, Houston; and Weill Cornell Medical College, New York, New York.
出版信息
Arch Pathol Lab Med. 2016 Apr;140(4):312-7. doi: 10.5858/arpa.2015-0361-OA. Epub 2015 Oct 2.
CONTEXT
The classification of pulmonary large cell carcinoma has undergone a major revision with the recent World Health Organization (WHO) 2015 Classification. Many large cell carcinomas are now reassigned to either adenocarcinoma with solid pattern or nonkeratinizing squamous cell carcinoma based on immunopositivity for adenocarcinoma markers or squamous cell carcinoma markers, respectively. Large cell carcinomas that are negative for adenocarcinoma and squamous cell carcinoma immunomarkers are now classified as large cell carcinoma with null immunohistochemical features (LCC-N). Although a few studies investigated the mutation profile of large cell carcinomas grouped by immunostain profile before the publication of the new WHO classification, investigation of tumors previously diagnosed as large cell carcinoma and reclassified according to the 2015 WHO classification has not, to our knowledge, been reported.
OBJECTIVE
To determine the mutation profiles of pulmonary large cell carcinomas reclassified by WHO 2015 criteria.
DESIGN
Archival cases of non-small cell lung carcinoma with large cell carcinoma morphology (n = 17) were reclassified according to 2015 WHO criteria. To determine mutation profile, we employed Ion Torrent (Life Technologies, Carlsbad, California)-based next-generation sequencing (50 genes; more than 2800 mutations) in addition to real-time quantitative reverse transcription polymerase chain reaction for ALK translocation detection.
RESULTS
Two of 17 cases (12%) were reclassified as LCC-N, and both had mutations-BRAF D594N in one case and KRAS G12C in the other case. Seven of 17 cases (41%) were reclassified in the adenocarcinoma with solid pattern group, which showed one KRAS G12C and one EGFR E709K + G719C double mutation in addition to mutations in TP53. Eight of 17 cases (47%) were reclassified in the nonkeratinizing squamous cell carcinoma group, which showed mutations in PIK3CA, CDKN2A, and TP53. No ALK translocations or amplifications were detected.
CONCLUSIONS
The adenocarcinoma with solid pattern group showed mutations typical of adenocarcinoma, whereas the nonkeratinizing squamous cell carcinoma group showed mutations typical of squamous cell carcinoma. Both LCC-N cases had mutations associated with adenocarcinoma, supporting the hypothesis that LCC-N is related to adenocarcinoma.
背景
随着世界卫生组织(WHO)2015年分类标准的发布,肺大细胞癌的分类发生了重大修订。现在,许多大细胞癌分别根据腺癌标志物或鳞状细胞癌标志物的免疫阳性结果,重新归类为实性型腺癌或非角化性鳞状细胞癌。对腺癌和鳞状细胞癌免疫标志物均呈阴性的大细胞癌,现在被归类为无免疫组化特征的大细胞癌(LCC-N)。尽管在新的WHO分类标准发布之前,有一些研究调查了按免疫染色特征分组的大细胞癌的突变谱,但据我们所知,尚未有关于对先前诊断为大细胞癌并根据2015年WHO分类标准重新分类的肿瘤的研究报道。
目的
确定根据WHO 2015标准重新分类的肺大细胞癌的突变谱。
设计
对17例具有大细胞癌形态的非小细胞肺癌存档病例,根据2015年WHO标准进行重新分类。为了确定突变谱,我们采用基于Ion Torrent(美国加利福尼亚州卡尔斯巴德市Life Technologies公司)的新一代测序技术(检测50个基因;超过2800个突变),并结合实时定量逆转录聚合酶链反应检测ALK易位。
结果
17例病例中有2例(12%)被重新归类为LCC-N,其中1例有BRAF D594N突变,另1例有KRAS G12C突变。17例病例中有7例(41%)被重新归类到实性型腺癌组,除TP53突变外,还显示1例KRAS G12C突变和1例EGFR E709K + G719C双突变。17例病例中有8例(47%)被重新归类到非角化性鳞状细胞癌组,显示PIK3CA、CDKN2A和TP53突变。未检测到ALK易位或扩增。
结论
实性型腺癌组显示出腺癌典型的突变,而非角化性鳞状细胞癌组显示出鳞状细胞癌典型的突变。两例LCC-N病例均有与腺癌相关的突变,支持LCC-N与腺癌相关的假说。
Zotero 插件