肺癌
靶向治疗
外显子
外显子跳跃
医学
肿瘤科
癌症研究
病态的
癌症
内科学
生物信息学
生物
遗传学
基因
选择性拼接
作者
Ruichao Chai,Xing Liu,Bo Pang,Yu‐Qing Liu,Jingjun Li,Yang‐Fang Li,Zheng Zhao,Jiang Du,Zhaoshi Bao,Tao Jiang
摘要
Identifying molecular features is an essential component of the management and targeted therapy of brain metastases (BMs). The molecular features are different between primary lung cancers and BMs of lung cancer. Here we report the DNA and RNA mutational profiles of 43 pathological samples of BMs. In addition to previously reported mutational events associated with targeted therapy, PTPRZ1-MET, which was previously exclusively identified in glioma, was present in two cases of BMs of lung cancer. Furthermore, MET exon 14 skipping may be more common (6/37 cases) in BMs of lung cancer than the frequency previously reported in lung cancer. These findings highlight the clinical significance of targeted DNA plus RNA sequencing for BMs and suggest PTPRZ1-MET and MET exon 14 skipping as critical molecular events that may serve as targets of targeted therapy in BMs.
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