Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4

BACKGROUND: Fifty percent of lung adenocarcinomas harbor somatic mutations in six genes that encode proteins in the EGFR signaling pathway, i.e., EGFR, HER2/ERBB2, HER4/ERBB4, PIK3CA, BRAF, and KRAS. We performed mutational profiling of a large cohort of lung adenocarcinomas to uncover other potenti...

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Autores principales: Marks, Jenifer L., McLellan, Michael D., Zakowski, Maureen F., Lash, Alex E., Kasai, Yumi, Broderick, Stephen, Sarkaria, Inderpal S., Pham, DuyKhanh, Singh, Bhuvanesh, Miner, Tracie L., Fewell, Ginger A., Fulton, Lucinda L., Mardis, Elaine R., Wilson, Richard K., Kris, Mark G., Rusch, Valerie W., Varmus, Harold, Pao, William
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2007
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1855985/
https://www.ncbi.nlm.nih.gov/pubmed/17487277
http://dx.doi.org/10.1371/journal.pone.0000426
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author Marks, Jenifer L.
McLellan, Michael D.
Zakowski, Maureen F.
Lash, Alex E.
Kasai, Yumi
Broderick, Stephen
Sarkaria, Inderpal S.
Pham, DuyKhanh
Singh, Bhuvanesh
Miner, Tracie L.
Fewell, Ginger A.
Fulton, Lucinda L.
Mardis, Elaine R.
Wilson, Richard K.
Kris, Mark G.
Rusch, Valerie W.
Varmus, Harold
Pao, William
author_facet Marks, Jenifer L.
McLellan, Michael D.
Zakowski, Maureen F.
Lash, Alex E.
Kasai, Yumi
Broderick, Stephen
Sarkaria, Inderpal S.
Pham, DuyKhanh
Singh, Bhuvanesh
Miner, Tracie L.
Fewell, Ginger A.
Fulton, Lucinda L.
Mardis, Elaine R.
Wilson, Richard K.
Kris, Mark G.
Rusch, Valerie W.
Varmus, Harold
Pao, William
author_sort Marks, Jenifer L.
collection PubMed
description BACKGROUND: Fifty percent of lung adenocarcinomas harbor somatic mutations in six genes that encode proteins in the EGFR signaling pathway, i.e., EGFR, HER2/ERBB2, HER4/ERBB4, PIK3CA, BRAF, and KRAS. We performed mutational profiling of a large cohort of lung adenocarcinomas to uncover other potential somatic mutations in genes of this signaling pathway that could contribute to lung tumorigenesis. METHODOLOGY/PRINCIPAL FINDINGS: We analyzed genomic DNA from a total of 261 resected, clinically annotated non-small cell lung cancer (NSCLC) specimens. The coding sequences of 39 genes were screened for somatic mutations via high-throughput dideoxynucleotide sequencing of PCR-amplified gene products. Mutations were considered to be somatic only if they were found in an independent tumor-derived PCR product but not in matched normal tissue. Sequencing of 9MB of tumor sequence identified 239 putative genetic variants. We further examined 22 variants found in RAS family genes and 135 variants localized to exons encoding the kinase domain of respective proteins. We identified a total of 37 non-synonymous somatic mutations; 36 were found collectively in EGFR, KRAS, BRAF, and PIK3CA. One somatic mutation was a previously unreported mutation in the kinase domain (exon 16) of FGFR4 (Glu681Lys), identified in 1 of 158 tumors. The FGFR4 mutation is analogous to a reported tumor-specific somatic mutation in ERBB2 and is located in the same exon as a previously reported kinase domain mutation in FGFR4 (Pro712Thr) in a lung adenocarcinoma cell line. CONCLUSIONS/SIGNIFICANCE: This study is one of the first comprehensive mutational analyses of major genes in a specific signaling pathway in a sizeable cohort of lung adenocarcinomas. Our results suggest the majority of gain-of-function mutations within kinase genes in the EGFR signaling pathway have already been identified. Our findings also implicate FGFR4 in the pathogenesis of a subset of lung adenocarcinomas.
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spelling pubmed-18559852007-05-09 Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4 Marks, Jenifer L. McLellan, Michael D. Zakowski, Maureen F. Lash, Alex E. Kasai, Yumi Broderick, Stephen Sarkaria, Inderpal S. Pham, DuyKhanh Singh, Bhuvanesh Miner, Tracie L. Fewell, Ginger A. Fulton, Lucinda L. Mardis, Elaine R. Wilson, Richard K. Kris, Mark G. Rusch, Valerie W. Varmus, Harold Pao, William PLoS One Research Article BACKGROUND: Fifty percent of lung adenocarcinomas harbor somatic mutations in six genes that encode proteins in the EGFR signaling pathway, i.e., EGFR, HER2/ERBB2, HER4/ERBB4, PIK3CA, BRAF, and KRAS. We performed mutational profiling of a large cohort of lung adenocarcinomas to uncover other potential somatic mutations in genes of this signaling pathway that could contribute to lung tumorigenesis. METHODOLOGY/PRINCIPAL FINDINGS: We analyzed genomic DNA from a total of 261 resected, clinically annotated non-small cell lung cancer (NSCLC) specimens. The coding sequences of 39 genes were screened for somatic mutations via high-throughput dideoxynucleotide sequencing of PCR-amplified gene products. Mutations were considered to be somatic only if they were found in an independent tumor-derived PCR product but not in matched normal tissue. Sequencing of 9MB of tumor sequence identified 239 putative genetic variants. We further examined 22 variants found in RAS family genes and 135 variants localized to exons encoding the kinase domain of respective proteins. We identified a total of 37 non-synonymous somatic mutations; 36 were found collectively in EGFR, KRAS, BRAF, and PIK3CA. One somatic mutation was a previously unreported mutation in the kinase domain (exon 16) of FGFR4 (Glu681Lys), identified in 1 of 158 tumors. The FGFR4 mutation is analogous to a reported tumor-specific somatic mutation in ERBB2 and is located in the same exon as a previously reported kinase domain mutation in FGFR4 (Pro712Thr) in a lung adenocarcinoma cell line. CONCLUSIONS/SIGNIFICANCE: This study is one of the first comprehensive mutational analyses of major genes in a specific signaling pathway in a sizeable cohort of lung adenocarcinomas. Our results suggest the majority of gain-of-function mutations within kinase genes in the EGFR signaling pathway have already been identified. Our findings also implicate FGFR4 in the pathogenesis of a subset of lung adenocarcinomas. Public Library of Science 2007-05-09 /pmc/articles/PMC1855985/ /pubmed/17487277 http://dx.doi.org/10.1371/journal.pone.0000426 Text en Marks et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Marks, Jenifer L.
McLellan, Michael D.
Zakowski, Maureen F.
Lash, Alex E.
Kasai, Yumi
Broderick, Stephen
Sarkaria, Inderpal S.
Pham, DuyKhanh
Singh, Bhuvanesh
Miner, Tracie L.
Fewell, Ginger A.
Fulton, Lucinda L.
Mardis, Elaine R.
Wilson, Richard K.
Kris, Mark G.
Rusch, Valerie W.
Varmus, Harold
Pao, William
Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4
title Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4
title_full Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4
title_fullStr Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4
title_full_unstemmed Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4
title_short Mutational Analysis of EGFR and Related Signaling Pathway Genes in Lung Adenocarcinomas Identifies a Novel Somatic Kinase Domain Mutation in FGFR4
title_sort mutational analysis of egfr and related signaling pathway genes in lung adenocarcinomas identifies a novel somatic kinase domain mutation in fgfr4
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1855985/
https://www.ncbi.nlm.nih.gov/pubmed/17487277
http://dx.doi.org/10.1371/journal.pone.0000426
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