中国人群肺腺癌中新型 NRG1、EGFR 和 MET 融合基因的检测。
Detection of Novel NRG1, EGFR, and MET Fusions in Lung Adenocarcinomas in the Chinese Population.
机构信息
Department of Thoracic Surgery, Fudan University Shanghai Cancer Center, Shanghai, China; Department of Pathology, Fudan University Shanghai Cancer Center, Shanghai, China.
Department of Oncology, Shanghai Medical College, Fudan University, Shanghai, China; Department of Pathology, Fudan University Shanghai Cancer Center, Shanghai, China.
出版信息
J Thorac Oncol. 2019 Nov;14(11):2003-2008. doi: 10.1016/j.jtho.2019.07.022. Epub 2019 Aug 2.
INTRODUCTION
Multiple oncogene fusions beyond ALK receptor tyrosine kinase (ALK), RET, and ROS1 fusion has been described in lung cancer, especially in lung adenocarcinomas without common oncogenic mutations. Molecular inhibitors have been developed and proved effective for patients whose tumors harbor these novel alterations.
METHODS
A consecutive series of surgically resected lung adenocarcinomas were collected and profiled using an enrichment strategy to detect nine common oncogenic driver mutations and fusions concerning EGFR, KRAS, HER2, BRAF, MET, ALK, RET, ROS1, and FGFR. Driver-negative cases were further analyzed by a comprehensive RNA-based next-generation sequencing (NGS) fusion assay for novel fusions.
RESULTS
In total, we profiled 1681 lung adenocarcinomas, among which 255 cases were common driver-negative. One hundred seventy-seven cases had sufficient tissue for NGS fusions screening, which identified eight novel fusions. NRG1 fusions occurred in 0.36% of all lung adenocarcinoma cases (6 of 1681 cases), including 4 CD74-NRG1-positive cases, 1 RBPMS-NRG1-positive case, and 1 novel ITGB1-NRG1-positive case. Furthermore, another 2 novel fusions were also detected, including 1 EGFR-SHC1 fusion and 1 CD47-MET fusion, both of which were in-frame and retained the functional domain of the corresponding kinases. No fusion event was detected for NTRK, KRAS, BRAF or HER2 genes in this cohort. Detailed clinicopathologic data showed that invasive mucous adenocarcinoma (three of eight cases) and acinar-predominant adenocarcinoma (three of eight cases) were the most prevalent pathologic subtypes among novel fusions.
CONCLUSIONS
Fusions affecting NRG1, EGFR, and MET were detected in 0.48% of unselected lung adenocarcinomas, and NRG1 fusions ranked the most prevalent fusions in common driver-negative lung adenocarcinomas from Chinese population. RNA-based NGS fusion assay was an optional method for screening actionable fusions in common driver-negative cases.
简介
除了 ALK 受体酪氨酸激酶 (ALK)、RET 和 ROS1 融合之外,在肺癌中已经描述了多种癌基因融合,尤其是在没有常见致癌突变的肺腺癌中。已经开发出针对这些新型改变的肿瘤的分子抑制剂,并已证明对患者有效。
方法
连续收集了一系列手术切除的肺腺癌,使用富集策略进行了分析,以检测涉及 EGFR、KRAS、HER2、BRAF、MET、ALK、RET、ROS1 和 FGFR 的九个常见致癌驱动突变和融合。对无常见驱动突变的病例,进一步通过全面的基于 RNA 的下一代测序 (NGS) 融合检测进行新型融合分析。
结果
总共分析了 1681 例肺腺癌,其中 255 例为常见的无驱动突变病例。177 例有足够的组织进行 NGS 融合筛选,发现了 8 种新型融合。NRG1 融合发生在所有肺腺癌病例的 0.36%(1681 例中的 6 例),包括 4 例 CD74-NRG1 阳性病例、1 例 RBPMS-NRG1 阳性病例和 1 例新型 ITGB1-NRG1 阳性病例。此外,还检测到另外 2 种新型融合,包括 1 例 EGFR-SHC1 融合和 1 例 CD47-MET 融合,两者均为框架内融合,保留了相应激酶的功能域。在该队列中未检测到 NTRK、KRAS、BRAF 或 HER2 基因的融合事件。详细的临床病理数据显示,浸润性黏液腺癌(8 例中的 3 例)和腺泡为主型腺癌(8 例中的 3 例)是新型融合中最常见的病理亚型。
结论
在未选择的肺腺癌中,检测到影响 NRG1、EGFR 和 MET 的融合,在来自中国人群的无常见驱动突变肺腺癌中,NRG1 融合是最常见的融合。基于 RNA 的 NGS 融合检测是筛选无常见驱动突变病例中可操作融合的一种可选方法。
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