GCC2-ALK as a targetable fusion in lung adenocarcinoma and its enduring clinical responses to ALK inhibitors

克里唑蒂尼 医学 腺癌 肺癌 肿瘤科 癌症 内科学 恶性胸腔积液
作者
Junhong Jiang,Xue Wu,Xiaoling Tong,Wangzhi Wei,Anan Chen,Xiaonan Wang,Yang Shao,Jianan Huang
出处
期刊:Lung Cancer [Elsevier BV]
卷期号:115: 5-11 被引量:29
标识
DOI:10.1016/j.lungcan.2017.10.011
摘要

Objectives ALK, RET and ROS1 fusions have been identified as treatable targets in 5%–15% of non-small-cell lung cancers, and thanks to the advanced sequencing technologies, their new partner genes have been steadily detected. Here we identified a rare fusion of ALK (GCC2-ALK) in a patient with advanced lung adenocarcinoma and monitored the treatment efficacy of ALK inhibitors on this patient. We further performed in vitro functional studies of this fusion protein for evaluating its oncogenic potential. Materials and methods The GCC2-ALK fusion gene was identified by targeted next generation sequencing (NGS) from the tumor DNA samples, and its fusion product was confirmed by Sanger sequencing the cDNA product. The functional study of GCC2-ALK was performed in Ba/F3 cells with cell proliferation and viability assays. The activation of downstream signaling pathways of ALK and their responses to crizotinib inhibition were studied in HEK-293 and 293T cells with ectopic expression of GCC2-ALK. In parallel, disease progression in the patient was monitored by computed tomography scanning and targeted NGS of either liquid or tissue biopsy samples throughout and after crizotinib treatment. Results Similarly to EML4-ALK, the GCC2-ALK fusion protein promotes IL-3-independent growth of Ba/F3 cells. Ectopic expression of GCC2-ALK leads to hyper-activation of ALK downstream signaling that can be inhibited by crizotinib. Crizotinib treatment of the patient resulted in 18 months of progression free survival without any trace of GCC2-ALK fusion in the liquid biopsies. Re-biopsy of a lung lesion at progression identified the re-occurrence of GCC2-ALK. The patient was then administrated with a second-generation ALK inhibitor, ceritinib, and received partial response until the last follow-up. Conclusion We identified and functionally validated GCC2-ALK as a constitutively activated fusion in NSCLC. The patient was benefited from crizotinib treatment initially and then ceritinib after progression, suggesting GCC2-ALK as a novel therapeutic target for ALK inhibitors.

科研通智能强力驱动
Strongly Powered by AbleSci AI
科研通是完全免费的文献互助平台,具备全网最快的应助速度,最高的求助完成率。 对每一个文献求助,科研通都将尽心尽力,给求助人一个满意的交代。
实时播报
悦耳扬完成签到,获得积分10
刚刚
星星国王完成签到,获得积分10
1秒前
hi发布了新的文献求助10
1秒前
1秒前
举人烧烤发布了新的文献求助10
2秒前
青衣完成签到,获得积分10
2秒前
chenqiang完成签到,获得积分10
2秒前
杜杨帆发布了新的文献求助10
3秒前
火星弟弟发布了新的文献求助10
3秒前
Jason是个大天才完成签到,获得积分10
3秒前
恬恬完成签到,获得积分10
4秒前
123123完成签到,获得积分10
4秒前
hu完成签到,获得积分10
4秒前
5秒前
情怀应助刻苦秋烟采纳,获得10
6秒前
andrew完成签到,获得积分10
6秒前
bioyong发布了新的文献求助10
6秒前
爆米花应助JR采纳,获得10
7秒前
hu发布了新的文献求助10
7秒前
7秒前
乐乐应助哈温采纳,获得10
7秒前
华仔应助gong采纳,获得10
8秒前
8秒前
科研通AI6.4应助123123采纳,获得10
8秒前
8秒前
逗逗关注了科研通微信公众号
9秒前
胡昱文发布了新的文献求助10
10秒前
Heisenberg完成签到,获得积分10
10秒前
小蘑菇应助xzn采纳,获得10
10秒前
ya完成签到,获得积分10
12秒前
YLi_746发布了新的文献求助10
12秒前
jason完成签到 ,获得积分10
13秒前
Dani完成签到,获得积分10
13秒前
过时的疾发布了新的文献求助10
14秒前
悦耳亦云完成签到 ,获得积分10
15秒前
斯文败类应助椰子采纳,获得10
15秒前
林岚完成签到,获得积分10
15秒前
15秒前
16秒前
16秒前
高分求助中
Principles of Economics, 11th Edition 10000
University Physics with Modern Physics, 16th edition 10000
(应助此贴封号)【重要!!请各用户(尤其是新用户)详细阅读】【科研通的精品贴汇总】 10000
48V Low-voltage Power Distribution Network (PDN) Architecture Industry Report, 2024 800
ズームレンズの光学設計に関する研究 800
Fundamentals of Pharmaceutical and Biologics Regulations: A Global Perspective, Second Edition 700
Matrix Methods in Data Mining and Pattern Recognition Second Edition 610
热门求助领域 (近24小时)
化学 材料科学 医学 生物 纳米技术 工程类 有机化学 化学工程 生物化学 计算机科学 内科学 物理 复合材料 催化作用 细胞生物学 无机化学 光电子学 物理化学 电极 基因
热门帖子
关注 科研通微信公众号,转发送积分 7300434
求助须知:如何正确求助?哪些是违规求助? 8918749
关于积分的说明 18888418
捐赠科研通 6965274
什么是DOI,文献DOI怎么找? 3211133
关于科研通互助平台的介绍 2380360
邀请新用户注册赠送积分活动 2187852