The contribution of hereditary cancer-related germline mutations to lung cancer susceptibility

Mengyuan Liu; Xinyi Liu; Peisu Suo; Yuan Gong; Baolin Qu; Xiumei Peng; Wenhua Xiao; Yuemin Li; Yan Chen; Zhen Zeng; Yinying Lu; Tanxiao Huang; Yingshen Zhao; Ming Liu; Lifeng Li; Yaru Chen; Yanqing Zhou; Guifeng Liu; Jianfei Yao; Shifu Chen; Lele Song

doi:10.21037/tlcr-19-403

The contribution of hereditary cancer-related germline mutations to lung cancer susceptibility

Transl Lung Cancer Res. 2020 Jun;9(3):646-658. doi: 10.21037/tlcr-19-403.

Authors

Mengyuan Liu¹, Xinyi Liu¹, Peisu Suo¹, Yuan Gong², Baolin Qu², Xiumei Peng³, Wenhua Xiao³, Yuemin Li⁴, Yan Chen⁵, Zhen Zeng⁵, Yinying Lu⁵, Tanxiao Huang¹, Yingshen Zhao¹, Ming Liu¹, Lifeng Li¹, Yaru Chen¹, Yanqing Zhou¹, Guifeng Liu¹, Jianfei Yao¹, Shifu Chen¹, Lele Song^{1

4}

Affiliations

¹ HaploX Biotechnology, Co., Ltd., Shenzhen 518057, China.
² The Second Medical Center of the Chinese PLA General Hospital, Beijing 100853, China.
³ The Fourth Medical Center of the Chinese PLA General Hospital, Beijing 100037, China.
⁴ The Eighth Medical Center of the Chinese PLA General Hospital, Beijing 100091, China.
⁵ The Fifth Medical Center of the Chinese PLA General Hospital, Beijing 100039, China.

Abstract

Background: Germline variations may contribute to lung cancer susceptibility besides environmental factors. The influence of germline mutations on lung cancer susceptibility and their correlation with somatic mutations has not been systematically investigated.

Methods: In this study, germline mutations from 1,026 non-small cell lung cancer (NSCLC) patients were analyzed with a 58-gene next-generation sequencing (NGS) panel containing known hereditary cancer-related genes, and were categorized based on American College of Medical Genetics and Genomics (ACMG) guidelines in pathogenicity, and the corresponding somatic mutations were analyzed using a 605-gene NGS panel containing known cancer-related genes.

Results: Plausible genetic susceptibility was found in 4.7% of lung cancer patients, in which 14 patients with pathogenic mutations (P group) and 34 patients with likely-pathogenic mutations (LP group) were identified. The ratio of the first degree relatives with lung cancer history of the P groups was significantly higher than the Non-P group (P=0.009). The ratio of lung cancer patients with history of other cancers was higher in P (P=0.0007) or LP (P=0.017) group than the Non-P group. Pathogenic mutations fell most commonly in BRCA2, followed by CHEK2 and ATM. Likely-pathogenic mutations fell most commonly in NTRK1 and EXT2, followed by BRIP1 and PALB2. These genes are involved in DNA repair, cell cycle regulation and tumor suppression. By comparing the germline mutation frequency from this study with that from the whole population or East Asian population (gnomAD database), we found that the overall odds ratio (OR) for P or LP group was 17.93 and 15.86, respectively, when compared with the whole population, and was 2.88 and 3.80, respectively, when compared with the East Asian population, suggesting the germline mutations of the P and LP groups were risk factors for lung cancer. Somatic mutation analysis revealed no significant difference in tumor mutation burden (TMB) among the groups, although a trend of lower TMB in the pathogenic group was found. The SNV/INDEL mutation frequency of TP53 in the P group was significantly lower than the other two groups, and the copy number variation (CNV) mutation frequency of PIK3CA and MET was significantly higher than the Non-P group. Pathway enrichment analysis found no significant difference in aberrant pathways among the three groups.

Conclusions: A proportion of 4.7% of patients carrying germline variants may be potentially linked to increased susceptibility to lung cancer. Patients with pathogenic germline mutations exhibited stronger family history and higher lung cancer risk.

Keywords: BRCA2; EGFR; Lung cancer; germline; pathogenic; susceptibility.