Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study

Jianxin Shi; Xing Hua; Bin Zhu; Sarangan Ravichandran; Mingyi Wang; Cu Nguyen; Seth A. Brodie; Alessandro Palleschi; Marco Alloisio; Gianluca Pariscenti; Kristine Jones; Weiyin Zhou; Aaron J. Bouk; Joseph Boland; Belynda Hicks; Adam Risch; Hunter Bennett; Brian T. Luke; Lei Song; Jubao Duan; Pengyuan Liu; Takashi Kohno; Qingrong Chen; Daoud Meerzaman; Crystal Marconett; Ite Laird-Offringa; Ian Mills; Neil E. Caporaso; Mitchell H. Gail; Angela C. Pesatori; Dario Consonni; Pier Alberto Bertazzi; Stephen J. Chanock; Maria Teresa Landi

doi:10.1371/journal.pmed.1002162

Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study

Jianxin Shi, Xing Hua, Bin Zhu, Sarangan Ravichandran, Mingyi Wang, Cu Nguyen, Seth A. Brodie, Alessandro Palleschi, Marco Alloisio, Gianluca Pariscenti, Kristine Jones, Weiyin Zhou, Aaron J. Bouk, Joseph Boland, Belynda Hicks, Adam Risch, Hunter Bennett, Brian T. Luke, Lei Song, Jubao DuanPengyuan Liu, Takashi Kohno, Qingrong Chen, Daoud Meerzaman, Crystal Marconett, Ite Laird-Offringa, Ian Mills, Neil E. Caporaso, Mitchell H. Gail, Angela C. Pesatori, Dario Consonni, Pier Alberto Bertazzi, Stephen J. Chanock, Maria Teresa Landi

School of Medicine

Research output: Contribution to journal › Article › peer-review

47 Scopus citations

Abstract

Background: Lung adenocarcinoma (LUAD) is the most common histologic subtype of lung cancer and has a high risk of distant metastasis at every disease stage. We aimed to characterize the genomic landscape of LUAD and identify mutation signatures associated with tumor progression. Methods and Findings: We performed an integrative genomic analysis, incorporating whole exome sequencing (WES), determination of DNA copy number and DNA methylation, and transcriptome sequencing for 101 LUAD samples from the Environment And Genetics in Lung cancer Etiology (EAGLE) study. We detected driver genes by testing whether the nonsynonymous mutation rate was significantly higher than the background mutation rate and replicated our findings in public datasets with 724 samples. We performed subclonality analysis for mutations based on mutant allele data and copy number alteration data. We also tested the association between mutation signatures and clinical outcomes, including distant metastasis, survival, and tumor grade. We identified and replicated two novel candidate driver genes, POU class 4 homeobox 2 (POU4F2) (mutated in 9 [8.9%] samples) and ZKSCAN1 (mutated in 6 [5.9%] samples), and characterized their major deleterious mutations. ZKSCAN1 was part of a mutually exclusive gene set that included the RTK/RAS/RAF pathway genes BRAF, EGFR, KRAS, MET, and NF1, indicating an important driver role for this gene. Moreover, we observed strong associations between methylation in specific genomic regions and somatic mutation patterns. In the tumor evolution analysis, four driver genes had a significantly lower fraction of subclonal mutations (FSM), including TP53 (p = 0.007), KEAP1 (p = 0.012), STK11 (p = 0.0076), and EGFR (p = 0.0078), suggesting a tumor initiation role for these genes. Subclonal mutations were significantly enriched in APOBEC-related signatures (p < 2.5×10⁻⁵⁰). The total number of somatic mutations (p = 0.0039) and the fraction of transitions (p = 5.5×10⁻⁴) were associated with increased risk of distant metastasis. Our study’s limitations include a small number of LUAD patients for subgroup analyses and a single-sample design for investigation of subclonality. Conclusions: These data provide a genomic characterization of LUAD pathogenesis and progression. The distinct clonal and subclonal mutation signatures suggest possible diverse carcinogenesis pathways for endogenous and exogenous exposures, and may serve as a foundation for more effective treatments for this lethal disease. LUAD’s high heterogeneity emphasizes the need to further study this tumor type and to associate genomic findings with clinical outcomes.

Original language	English (US)
Article number	e1002162
Journal	PLoS medicine
Volume	13
Issue number	12
DOIs	https://doi.org/10.1371/journal.pmed.1002162
State	Published - Dec 2016

ASJC Scopus subject areas

Medicine(all)

Access to Document

10.1371/journal.pmed.1002162

Cite this

Shi, J., Hua, X., Zhu, B., Ravichandran, S., Wang, M., Nguyen, C., Brodie, S. A., Palleschi, A., Alloisio, M., Pariscenti, G., Jones, K., Zhou, W., Bouk, A. J., Boland, J., Hicks, B., Risch, A., Bennett, H., Luke, B. T., Song, L., ... Landi, M. T. (2016). Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study. PLoS medicine, 13(12), [e1002162]. https://doi.org/10.1371/journal.pmed.1002162

Shi, J, Hua, X, Zhu, B, Ravichandran, S, Wang, M, Nguyen, C, Brodie, SA, Palleschi, A, Alloisio, M, Pariscenti, G, Jones, K, Zhou, W, Bouk, AJ, Boland, J, Hicks, B, Risch, A, Bennett, H, Luke, BT, Song, L, Duan, J, Liu, P, Kohno, T, Chen, Q, Meerzaman, D, Marconett, C, Laird-Offringa, I, Mills, I, Caporaso, NE, Gail, MH, Pesatori, AC, Consonni, D, Bertazzi, PA, Chanock, SJ & Landi, MT 2016, 'Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study', PLoS medicine, vol. 13, no. 12, e1002162. https://doi.org/10.1371/journal.pmed.1002162

@article{bc65c66eb51347299b1a168bad77eb22,

title = "Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study",

abstract = "Background: Lung adenocarcinoma (LUAD) is the most common histologic subtype of lung cancer and has a high risk of distant metastasis at every disease stage. We aimed to characterize the genomic landscape of LUAD and identify mutation signatures associated with tumor progression. Methods and Findings: We performed an integrative genomic analysis, incorporating whole exome sequencing (WES), determination of DNA copy number and DNA methylation, and transcriptome sequencing for 101 LUAD samples from the Environment And Genetics in Lung cancer Etiology (EAGLE) study. We detected driver genes by testing whether the nonsynonymous mutation rate was significantly higher than the background mutation rate and replicated our findings in public datasets with 724 samples. We performed subclonality analysis for mutations based on mutant allele data and copy number alteration data. We also tested the association between mutation signatures and clinical outcomes, including distant metastasis, survival, and tumor grade. We identified and replicated two novel candidate driver genes, POU class 4 homeobox 2 (POU4F2) (mutated in 9 [8.9%] samples) and ZKSCAN1 (mutated in 6 [5.9%] samples), and characterized their major deleterious mutations. ZKSCAN1 was part of a mutually exclusive gene set that included the RTK/RAS/RAF pathway genes BRAF, EGFR, KRAS, MET, and NF1, indicating an important driver role for this gene. Moreover, we observed strong associations between methylation in specific genomic regions and somatic mutation patterns. In the tumor evolution analysis, four driver genes had a significantly lower fraction of subclonal mutations (FSM), including TP53 (p = 0.007), KEAP1 (p = 0.012), STK11 (p = 0.0076), and EGFR (p = 0.0078), suggesting a tumor initiation role for these genes. Subclonal mutations were significantly enriched in APOBEC-related signatures (p < 2.5×10−50). The total number of somatic mutations (p = 0.0039) and the fraction of transitions (p = 5.5×10−4) were associated with increased risk of distant metastasis. Our study{\textquoteright}s limitations include a small number of LUAD patients for subgroup analyses and a single-sample design for investigation of subclonality. Conclusions: These data provide a genomic characterization of LUAD pathogenesis and progression. The distinct clonal and subclonal mutation signatures suggest possible diverse carcinogenesis pathways for endogenous and exogenous exposures, and may serve as a foundation for more effective treatments for this lethal disease. LUAD{\textquoteright}s high heterogeneity emphasizes the need to further study this tumor type and to associate genomic findings with clinical outcomes.",

author = "Jianxin Shi and Xing Hua and Bin Zhu and Sarangan Ravichandran and Mingyi Wang and Cu Nguyen and Brodie, {Seth A.} and Alessandro Palleschi and Marco Alloisio and Gianluca Pariscenti and Kristine Jones and Weiyin Zhou and Bouk, {Aaron J.} and Joseph Boland and Belynda Hicks and Adam Risch and Hunter Bennett and Luke, {Brian T.} and Lei Song and Jubao Duan and Pengyuan Liu and Takashi Kohno and Qingrong Chen and Daoud Meerzaman and Crystal Marconett and Ite Laird-Offringa and Ian Mills and Caporaso, {Neil E.} and Gail, {Mitchell H.} and Pesatori, {Angela C.} and Dario Consonni and Bertazzi, {Pier Alberto} and Chanock, {Stephen J.} and Landi, {Maria Teresa}",

year = "2016",

month = dec,

doi = "10.1371/journal.pmed.1002162",

language = "English (US)",

volume = "13",

journal = "PLoS Medicine",

issn = "1549-1277",

number = "12",

}

TY - JOUR

T1 - Somatic Genomics and Clinical Features of Lung Adenocarcinoma

T2 - A Retrospective Study

AU - Shi, Jianxin

AU - Hua, Xing

AU - Zhu, Bin

AU - Ravichandran, Sarangan

AU - Wang, Mingyi

AU - Nguyen, Cu

AU - Brodie, Seth A.

AU - Palleschi, Alessandro

AU - Alloisio, Marco

AU - Pariscenti, Gianluca

AU - Jones, Kristine

AU - Zhou, Weiyin

AU - Bouk, Aaron J.

AU - Boland, Joseph

AU - Hicks, Belynda

AU - Risch, Adam

AU - Bennett, Hunter

AU - Luke, Brian T.

AU - Song, Lei

AU - Duan, Jubao

AU - Liu, Pengyuan

AU - Kohno, Takashi

AU - Chen, Qingrong

AU - Meerzaman, Daoud

AU - Marconett, Crystal

AU - Laird-Offringa, Ite

AU - Mills, Ian

AU - Caporaso, Neil E.

AU - Gail, Mitchell H.

AU - Pesatori, Angela C.

AU - Consonni, Dario

AU - Bertazzi, Pier Alberto

AU - Chanock, Stephen J.

AU - Landi, Maria Teresa

PY - 2016/12

Y1 - 2016/12

N2 - Background: Lung adenocarcinoma (LUAD) is the most common histologic subtype of lung cancer and has a high risk of distant metastasis at every disease stage. We aimed to characterize the genomic landscape of LUAD and identify mutation signatures associated with tumor progression. Methods and Findings: We performed an integrative genomic analysis, incorporating whole exome sequencing (WES), determination of DNA copy number and DNA methylation, and transcriptome sequencing for 101 LUAD samples from the Environment And Genetics in Lung cancer Etiology (EAGLE) study. We detected driver genes by testing whether the nonsynonymous mutation rate was significantly higher than the background mutation rate and replicated our findings in public datasets with 724 samples. We performed subclonality analysis for mutations based on mutant allele data and copy number alteration data. We also tested the association between mutation signatures and clinical outcomes, including distant metastasis, survival, and tumor grade. We identified and replicated two novel candidate driver genes, POU class 4 homeobox 2 (POU4F2) (mutated in 9 [8.9%] samples) and ZKSCAN1 (mutated in 6 [5.9%] samples), and characterized their major deleterious mutations. ZKSCAN1 was part of a mutually exclusive gene set that included the RTK/RAS/RAF pathway genes BRAF, EGFR, KRAS, MET, and NF1, indicating an important driver role for this gene. Moreover, we observed strong associations between methylation in specific genomic regions and somatic mutation patterns. In the tumor evolution analysis, four driver genes had a significantly lower fraction of subclonal mutations (FSM), including TP53 (p = 0.007), KEAP1 (p = 0.012), STK11 (p = 0.0076), and EGFR (p = 0.0078), suggesting a tumor initiation role for these genes. Subclonal mutations were significantly enriched in APOBEC-related signatures (p < 2.5×10−50). The total number of somatic mutations (p = 0.0039) and the fraction of transitions (p = 5.5×10−4) were associated with increased risk of distant metastasis. Our study’s limitations include a small number of LUAD patients for subgroup analyses and a single-sample design for investigation of subclonality. Conclusions: These data provide a genomic characterization of LUAD pathogenesis and progression. The distinct clonal and subclonal mutation signatures suggest possible diverse carcinogenesis pathways for endogenous and exogenous exposures, and may serve as a foundation for more effective treatments for this lethal disease. LUAD’s high heterogeneity emphasizes the need to further study this tumor type and to associate genomic findings with clinical outcomes.

AB - Background: Lung adenocarcinoma (LUAD) is the most common histologic subtype of lung cancer and has a high risk of distant metastasis at every disease stage. We aimed to characterize the genomic landscape of LUAD and identify mutation signatures associated with tumor progression. Methods and Findings: We performed an integrative genomic analysis, incorporating whole exome sequencing (WES), determination of DNA copy number and DNA methylation, and transcriptome sequencing for 101 LUAD samples from the Environment And Genetics in Lung cancer Etiology (EAGLE) study. We detected driver genes by testing whether the nonsynonymous mutation rate was significantly higher than the background mutation rate and replicated our findings in public datasets with 724 samples. We performed subclonality analysis for mutations based on mutant allele data and copy number alteration data. We also tested the association between mutation signatures and clinical outcomes, including distant metastasis, survival, and tumor grade. We identified and replicated two novel candidate driver genes, POU class 4 homeobox 2 (POU4F2) (mutated in 9 [8.9%] samples) and ZKSCAN1 (mutated in 6 [5.9%] samples), and characterized their major deleterious mutations. ZKSCAN1 was part of a mutually exclusive gene set that included the RTK/RAS/RAF pathway genes BRAF, EGFR, KRAS, MET, and NF1, indicating an important driver role for this gene. Moreover, we observed strong associations between methylation in specific genomic regions and somatic mutation patterns. In the tumor evolution analysis, four driver genes had a significantly lower fraction of subclonal mutations (FSM), including TP53 (p = 0.007), KEAP1 (p = 0.012), STK11 (p = 0.0076), and EGFR (p = 0.0078), suggesting a tumor initiation role for these genes. Subclonal mutations were significantly enriched in APOBEC-related signatures (p < 2.5×10−50). The total number of somatic mutations (p = 0.0039) and the fraction of transitions (p = 5.5×10−4) were associated with increased risk of distant metastasis. Our study’s limitations include a small number of LUAD patients for subgroup analyses and a single-sample design for investigation of subclonality. Conclusions: These data provide a genomic characterization of LUAD pathogenesis and progression. The distinct clonal and subclonal mutation signatures suggest possible diverse carcinogenesis pathways for endogenous and exogenous exposures, and may serve as a foundation for more effective treatments for this lethal disease. LUAD’s high heterogeneity emphasizes the need to further study this tumor type and to associate genomic findings with clinical outcomes.

UR - http://www.scopus.com/inward/record.url?scp=85007551446&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85007551446&partnerID=8YFLogxK

U2 - 10.1371/journal.pmed.1002162

DO - 10.1371/journal.pmed.1002162

M3 - Article

C2 - 27923066

AN - SCOPUS:85007551446

SN - 1549-1277

VL - 13

JO - PLoS Medicine

JF - PLoS Medicine

IS - 12

M1 - e1002162

ER -

Somatic Genomics and Clinical Features of Lung Adenocarcinoma: A Retrospective Study

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this