Targeted deep sequencing from multiple sources demonstrates increased NOTCH1 alterations in lung cancer patient plasma

Yuwei Liao; Zhaokui Ma; Yu Zhang; Dan Li; Dekang Lv; Zhisheng Chen; Peiying Li; Aisha Ai-Dherasi; Feng Zheng; Jichao Tian; Kun Zou; Yue Wang; Dongxia Wang; Miguel Cordova; Huan Zhou; Xiuhua Li; Dan Liu; Ruofei Yu; Qingzheng Zhang; Xiaolong Zhang; Jian Zhang; Xuehong Zhang; Xia Zhang; Yulong Li; Yanyan Shao; Luyao Song; Ruimei Liu; Yichen Wang; Sufiyan Sufiyan; Quentin Liu; Gareth I Owen; Zhiguang Li; Jun Chen

doi:10.1002/cam4.2458

Targeted deep sequencing from multiple sources demonstrates increased NOTCH1 alterations in lung cancer patient plasma

Cancer Med. 2019 Sep;8(12):5673-5686. doi: 10.1002/cam4.2458. Epub 2019 Aug 1.

Authors

Yuwei Liao^{1

2}, Zhaokui Ma², Yu Zhang², Dan Li¹, Dekang Lv², Zhisheng Chen¹, Peiying Li², Aisha Ai-Dherasi², Feng Zheng³, Jichao Tian², Kun Zou⁴, Yue Wang¹, Dongxia Wang¹, Miguel Cordova⁵, Huan Zhou¹, Xiuhua Li¹, Dan Liu¹, Ruofei Yu¹, Qingzheng Zhang², Xiaolong Zhang², Jian Zhang², Xuehong Zhang², Xia Zhang², Yulong Li², Yanyan Shao², Luyao Song², Ruimei Liu², Yichen Wang², Sufiyan Sufiyan², Quentin Liu², Gareth I Owen⁵, Zhiguang Li^{2

6}, Jun Chen¹

Affiliations

¹ The Second Hospital of Dalian Medical University, Dalian, China.
² Center of Genome and Personalized Medicine, Institute of Cancer Stem Cell, Dalian Medical University, Dalian, China.
³ Advanced Institute for Medical Sciences, Dalian Medical University, Dalian, China.
⁴ The First Affiliated Hospital of Dalian Medical University, Dalian, China.
⁵ Faculty of Biological Sciences, Pontificia Universidad Católica de Chile, Santiago, Chile.
⁶ The Second Affiliated Hospital, School of Medicine, Zhengzhou University, Zhengzhou, China.

Abstract

Introduction: Targeted therapies are based on specific gene alterations. Various specimen types have been used to determine gene alterations, however, no systemic comparisons have yet been made. Herein, we assessed alterations in selected cancer-associated genes across varying sample sites in lung cancer patients.

Materials and methods: Targeted deep sequencing for 48 tumor-related genes was applied to 153 samples from 55 lung cancer patients obtained from six sources: Formalin-fixed paraffin-embedded (FFPE) tumor tissues, pleural effusion supernatant (PES) and pleural effusion cell sediments (PEC), white blood cells (WBCs), oral epithelial cells (OECs), and plasma.

Results: Mutations were detected in 96% (53/55) of the patients and in 83% (40/48) of the selected genes. Each sample type exhibited a characteristic mutational pattern. As anticipated, TP53 was the most affected sequence (54.5% patients), however this was followed by NOTCH1 (36%, across all sample types). EGFR was altered in patient samples at a frequency of 32.7% and KRAS 10.9%. This high EGFR/ low KRAS frequency is in accordance with other TCGA cohorts of Asian origin but differs from the Caucasian population where KRAS is the more dominant mutation. Additionally, 66% (31/47) of PEC samples had copy number variants (CNVs) in at least one gene. Unlike the concurrent loss and gain in most genes, herein NOTCH1 loss was identified in 21% patients, with no gain observed. Based on the relative prevalence of mutations and CNVs, we divided lung cancer patients into SNV-dominated, CNV-dominated, and codominated groups.

Conclusions: Our results confirm previous reports that EGFR mutations are more prevalent than KRAS in Chinese lung cancer patients. NOTCH1 gene alterations are more common than previously reported and reveals a role of NOTCH1 modifications in tumor metastasis. Furthermore, genetic material from malignant pleural effusion cell sediments may be a noninvasive manner to identify CNV and participate in treatment decisions.

Keywords: NOTCH1; lung cancer; next-generation sequencing; plasma; pleural effusion.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Carcinoma, Non-Small-Cell Lung / genetics*
DNA Copy Number Variations
High-Throughput Nucleotide Sequencing / methods*
Humans
Lung Neoplasms / genetics*
Mutation
Mutation Rate
Neoplasm Metastasis
Receptor, Notch1 / genetics*
Sequence Analysis, DNA

Substances

NOTCH1 protein, human
Receptor, Notch1

Abstract

Publication types

MeSH terms

Substances

Grants and funding