Validating a targeted next-generation sequencing assay and profiling somatic variants in Chinese non-small cell lung cancer patients

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作者
Ruirui Jiang
Bo Zhang
Xiaodong Teng
Peizhen Hu
Sanpeng Xu
Zuyu Zheng
Rui Liu
Tingdong Tang
Feng Ye
机构
[1] Sichuan University,Laboratory of Pathology, West China Hospital
[2] Sichuan University,Department of Pathology, West China Hospital
[3] The First Hospital of Lanzhou University,Department of Pathology
[4] Peking University Third Hospital,Department of Pathology
[5] Zhejiang University,Department of Pathology, The First Affiliated Hospital
[6] Air Force Medical University,Department of Pathology, Xijing Hospital
[7] Huazhong University of Science & Technology,Institute of Pathology, Tongji Hospital, Tongji Medical College
[8] Singlera Genomics Inc.,undefined
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Non-small cell lung cancer (NSCLC) is featured with complex genomic alterations. Molecular profiling of large cohort of NSCLC patients is thus a prerequisite for precision medicine. We first validated the detection performance of a next-generation sequencing (NGS) cancer hotspot panel, OncoAim, on formalin-fixed paraffin-embedded (FFPE) samples. We then utilized OncoAim to delineate the genomic aberrations in Chinese NSCLC patients. Overall detection performance was powerful for mutations with allele frequency (MAF) ≥ 5% at >500 × coverage depth, with >99% sensitivity, high specificity (positive predictive value > 99%), 94% accuracy and 96% repeatability. Profiling 422 NSCLC FFPE samples revealed that patient characteristics, including gender, age, lymphatic spread, histologic grade and histologic subtype were significantly associated with the mutation incidence of EGFR and TP53. Moreover, RTK signaling pathway activation was enriched in adenocarcinoma, while PI(3)K pathway activation, oxidative stress pathway activation, and TP53 pathway inhibition were more prevalent in squamous cell carcinoma. Additionally, novel co-existence (e.g., variants in BRAF and PTEN) and mutual-exclusiveness (e.g., alterations in EGFR and NFE2L2) were found. Finally, we revealed distinct mutation spectrum in TP53, as well as a previously undervalued PTEN aberration. Our findings could aid in improving diagnosis, prognosis and personalized therapeutic decisions of Chinese NSCLC patients.
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