Circulating Tumor DNA Mutation Profiling by Targeted Next Generation Sequencing Provides Guidance for Personalized Treatments in Multiple Cancer Types

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作者
Yongqian Shu
Xue Wu
Xiaoling Tong
Xiaonan Wang
Zhili Chang
Yu Mao
Xiaofeng Chen
Jing Sun
Zhenxin Wang
Zhuan Hong
Liangjun Zhu
Chunrong Zhu
Jun Chen
Ying Liang
Huawu Shao
Yang W. Shao
机构
[1] The First Affiliated Hospital of Nanjing Medical University,Jiangsu Province Hospital
[2] Geneseeq Technology Inc.,Department of Medical Oncology
[3] Nanjing Geneseeq Technology Inc.,Department of Chemoradiotherapy
[4] The First Affiliated Hospital of Soochow University,Department of Medical Oncology
[5] Jiangsu Institute of Cancer Research,Chengdu Institute of Biology
[6] Nanjing Medical University Affiliated Cancer Hospital,undefined
[7] Jiangsu Cancer Hospital,undefined
[8] Yinzhou Hospital Affiliated to Medical School of Ningbo University,undefined
[9] Sun Yat-sen University Cancer Centre,undefined
[10] State Key Laboratory of Oncology in South China,undefined
[11] Collaborative Innovation Centre for Cancer Medicine,undefined
[12] Chinese Academy of Sciences,undefined
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摘要
Cancer is a disease of complex genetic alterations, and comprehensive genetic diagnosis is beneficial to match each patient to appropriate therapy. However, acquisition of representative tumor samples is invasive and sometimes impossible. Circulating tumor DNA (ctDNA) is a promising tool to use as a non-invasive biomarker for cancer mutation profiling. Here we implemented targeted next generation sequencing (NGS) with a customized gene panel of 382 cancer-relevant genes on 605 ctDNA samples in multiple cancer types. Overall, tumor-specific mutations were identified in 87% of ctDNA samples, with mutation spectra highly concordant with their matched tumor tissues. 71% of patients had at least one clinically-actionable mutation, 76% of which have suggested drugs approved or in clinical trials. In particular, our study reveals a unique mutation spectrum in Chinese lung cancer patients which could be used to guide treatment decisions and monitor drug-resistant mutations. Taken together, our study demonstrated the feasibility of clinically-useful targeted NGS-based ctDNA mutation profiling to guide treatment decisions in cancer.
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