Concomitant resistance mechanisms to multiple tyrosine kinase inhibitors in ALK-positive non-small cell lung cancer

克里唑蒂尼 医学 肺癌 相伴的 癌症研究 酪氨酸激酶 酪氨酸激酶抑制剂 癌症 内科学 间变性淋巴瘤激酶 碱性抑制剂 肿瘤科 受体 恶性胸腔积液
作者
Yongfeng Yu,Qiuxiang Ou,Xue Wu,Hairong Bao,Yan Ding,Yang Shao,Shun Lü
出处
期刊:Lung Cancer [Elsevier BV]
卷期号:127: 19-24 被引量:49
标识
DOI:10.1016/j.lungcan.2018.11.024
摘要

ALK tyrosine kinase inhibitors (TKIs), including crizotinib and several next generation TKIs, have demonstrated beneficial clinical outcomes in ALK-positive non-small cell lung cancer (NSCLC). However, resistance mechanisms following multiple TKI treatments in ALK-positive NSCLC are not fully elucidated.Mutation profiles of 422 cancer-relevant genes in 52 patients with post-TKI biopsy samples were analyzed using next-generation sequencing (NGS), and compared between patients receiving crizotinib alone (n = 35) and multi-TKIs (n = 17).EML4-ALK variant 3 is the most frequent ALK variants in this cohort, followed by EML4-ALK variant 1. Half of the patients harbored ALK activating mutations upon progression on crizotinib treatment. After multi-TKIs treatment, 59% of the cases developed resistant ALK mutations, and concomitant ALK activating mutations were more commonly observed in this cohort (P = 0.031). Specifically, ALK G1269 A, L1196 M, and C1156Y substitutions were more common in crizotinib-alone samples, while ALK G1202R was significantly more enriched post-multi-TKIs (P = 0.009). Activated bypass signaling tended to be more prevalent in patients post-multi-TKIs. Furthermore, dual activation of ALK and bypass signaling was more frequently found in the multi-TKIs group (5/17, 29%) in contrast to crizotinib-alone (2/35, 6%) (P = 0.031). Additionally, concurrent TP53 mutation demonstrated significantly shorter progression-free survival (PFS) compared with TP53 wildtype in crizotinib-alone group (median PFS: 8 vs 13 months, Hazard Ratio = 1.494, P = 0.019).Concurrent ALK activating mutations and/or upregulated bypass signaling are more enriched in patients undergoing multiple ALK TKI treatments compared to crizotinib alone. Concomitant TP53 mutation correlated to unfavorable survival when receiving a single TKI crizotinib.
最长约 10秒,即可获得该文献文件

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
lifuyi291发布了新的文献求助10
1秒前
wqwq69完成签到,获得积分10
2秒前
Sea_U完成签到,获得积分0
2秒前
崔鹤然完成签到,获得积分10
3秒前
岩岩岩完成签到,获得积分10
4秒前
无敌大番茄完成签到,获得积分10
4秒前
糖糖科研顺利呀完成签到 ,获得积分10
5秒前
123完成签到,获得积分10
5秒前
小马甲应助大气的雁桃采纳,获得10
5秒前
飞鹰完成签到,获得积分10
6秒前
今夜不设防完成签到,获得积分10
7秒前
闫123完成签到,获得积分10
7秒前
杨帆完成签到,获得积分10
7秒前
剁手党完成签到,获得积分10
7秒前
wennuan0913完成签到 ,获得积分10
7秒前
虚幻的诗槐完成签到 ,获得积分10
8秒前
lihan含完成签到 ,获得积分10
8秒前
9秒前
天真白猫完成签到,获得积分10
9秒前
HH完成签到 ,获得积分10
9秒前
清脆初晴发布了新的文献求助50
10秒前
小栗完成签到,获得积分10
11秒前
陈秋艳完成签到,获得积分20
12秒前
hao完成签到,获得积分10
13秒前
13秒前
piu完成签到,获得积分20
13秒前
搞怪的服饰完成签到,获得积分10
13秒前
Hello应助天晴色烟雨采纳,获得10
14秒前
维修师傅完成签到,获得积分10
14秒前
dxt完成签到,获得积分10
15秒前
15秒前
allenice发布了新的文献求助30
15秒前
123完成签到,获得积分10
15秒前
YYQX完成签到,获得积分10
15秒前
无奈谷芹完成签到 ,获得积分10
16秒前
thinking完成签到,获得积分10
16秒前
欣喜的真发布了新的文献求助10
17秒前
做我所做完成签到 ,获得积分10
18秒前
无花果应助luyun采纳,获得10
18秒前
Redinn完成签到,获得积分10
18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
Molecular Mechanisms of Photosynthesis, 4th Edition 1000
Organic Reactions, Volume 116 1000
Current concepts in cutaneous toxicity : proceedings of the Fourth Conference on Cutaneous Toxicity, Washington, D.C., May 9-11, 1979 1000
The recovery-stress questionnaires : user manual 800
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 7257809
求助须知:如何正确求助?哪些是违规求助? 8879654
关于积分的说明 18758068
捐赠科研通 6938139
什么是DOI,文献DOI怎么找? 3201148
关于科研通互助平台的介绍 2375264
邀请新用户注册赠送积分活动 2176997