MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression

Asbestos-related lung cancer accounts for 4–12% of lung cancers worldwide. We have previously identified ADAM28 as a putative oncogene involved in asbestos-related lung adenocarcinoma (ARLC-AC). We hypothesised that similarly gene expression profiling of asbestos-related lung squamous cell carcinoma...

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Autores principales: Wright, Casey M., Savarimuthu Francis, Santiyagu M., Tan, Maxine E., Martins, Maria U., Winterford, Clay, Davidson, Morgan R., Duhig, Edwina E., Clarke, Belinda E., Hayward, Nicholas K., Yang, Ian A., Bowman, Rayleen V., Fong, Kwun M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3325913/
https://www.ncbi.nlm.nih.gov/pubmed/22514692
http://dx.doi.org/10.1371/journal.pone.0034943
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author Wright, Casey M.
Savarimuthu Francis, Santiyagu M.
Tan, Maxine E.
Martins, Maria U.
Winterford, Clay
Davidson, Morgan R.
Duhig, Edwina E.
Clarke, Belinda E.
Hayward, Nicholas K.
Yang, Ian A.
Bowman, Rayleen V.
Fong, Kwun M.
author_facet Wright, Casey M.
Savarimuthu Francis, Santiyagu M.
Tan, Maxine E.
Martins, Maria U.
Winterford, Clay
Davidson, Morgan R.
Duhig, Edwina E.
Clarke, Belinda E.
Hayward, Nicholas K.
Yang, Ian A.
Bowman, Rayleen V.
Fong, Kwun M.
author_sort Wright, Casey M.
collection PubMed
description Asbestos-related lung cancer accounts for 4–12% of lung cancers worldwide. We have previously identified ADAM28 as a putative oncogene involved in asbestos-related lung adenocarcinoma (ARLC-AC). We hypothesised that similarly gene expression profiling of asbestos-related lung squamous cell carcinomas (ARLC-SCC) may identify candidate oncogenes for ARLC-SCC. We undertook a microarray gene expression study in 56 subjects; 26 ARLC-SCC (defined as lung asbestos body (AB) counts >20AB/gram wet weight (gww) and 30 non-asbestos related lung squamous cell carcinoma (NARLC-SCC; no detectable lung asbestos bodies; 0AB/gww). Microarray and bioinformatics analysis identified six candidate genes differentially expressed between ARLC-SCC and NARLC-SCC based on statistical significance (p<0.001) and fold change (FC) of >2-fold. Two genes MS4A1 and CARD18, were technically replicated by qRT-PCR and showed consistent directional changes. As we also found MS4A1 to be overexpressed in ARLC-ACs, we selected this gene for biological validation in independent test sets (one internal, and one external dataset (2 primary tumor sets)). MS4A1 RNA expression dysregulation was validated in the external dataset but not in our internal dataset, likely due to the small sample size in the test set as immunohistochemical (IHC) staining for MS4A1 (CD20) showed that protein expression localized predominantly to stromal lymphocytes rather than tumor cells in ARLC-SCC. We conclude that differential expression of MS4A1 in this comparative gene expression study of ARLC-SCC versus NARLC-SCC is a stromal signal of uncertain significance, and an example of the rationale for tumor cell enrichment in preparation for gene expression studies where the aim is to identify markers of particular tumor phenotypes. Finally, our study failed to identify any strong gene candidates whose expression serves as a marker of asbestos etiology. Future research is required to determine the role of stromal lymphocyte MS4A1 dysregulation in pulmonary SCCs caused by asbestos.
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spelling pubmed-33259132012-04-18 MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression Wright, Casey M. Savarimuthu Francis, Santiyagu M. Tan, Maxine E. Martins, Maria U. Winterford, Clay Davidson, Morgan R. Duhig, Edwina E. Clarke, Belinda E. Hayward, Nicholas K. Yang, Ian A. Bowman, Rayleen V. Fong, Kwun M. PLoS One Research Article Asbestos-related lung cancer accounts for 4–12% of lung cancers worldwide. We have previously identified ADAM28 as a putative oncogene involved in asbestos-related lung adenocarcinoma (ARLC-AC). We hypothesised that similarly gene expression profiling of asbestos-related lung squamous cell carcinomas (ARLC-SCC) may identify candidate oncogenes for ARLC-SCC. We undertook a microarray gene expression study in 56 subjects; 26 ARLC-SCC (defined as lung asbestos body (AB) counts >20AB/gram wet weight (gww) and 30 non-asbestos related lung squamous cell carcinoma (NARLC-SCC; no detectable lung asbestos bodies; 0AB/gww). Microarray and bioinformatics analysis identified six candidate genes differentially expressed between ARLC-SCC and NARLC-SCC based on statistical significance (p<0.001) and fold change (FC) of >2-fold. Two genes MS4A1 and CARD18, were technically replicated by qRT-PCR and showed consistent directional changes. As we also found MS4A1 to be overexpressed in ARLC-ACs, we selected this gene for biological validation in independent test sets (one internal, and one external dataset (2 primary tumor sets)). MS4A1 RNA expression dysregulation was validated in the external dataset but not in our internal dataset, likely due to the small sample size in the test set as immunohistochemical (IHC) staining for MS4A1 (CD20) showed that protein expression localized predominantly to stromal lymphocytes rather than tumor cells in ARLC-SCC. We conclude that differential expression of MS4A1 in this comparative gene expression study of ARLC-SCC versus NARLC-SCC is a stromal signal of uncertain significance, and an example of the rationale for tumor cell enrichment in preparation for gene expression studies where the aim is to identify markers of particular tumor phenotypes. Finally, our study failed to identify any strong gene candidates whose expression serves as a marker of asbestos etiology. Future research is required to determine the role of stromal lymphocyte MS4A1 dysregulation in pulmonary SCCs caused by asbestos. Public Library of Science 2012-04-13 /pmc/articles/PMC3325913/ /pubmed/22514692 http://dx.doi.org/10.1371/journal.pone.0034943 Text en Wright 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
Wright, Casey M.
Savarimuthu Francis, Santiyagu M.
Tan, Maxine E.
Martins, Maria U.
Winterford, Clay
Davidson, Morgan R.
Duhig, Edwina E.
Clarke, Belinda E.
Hayward, Nicholas K.
Yang, Ian A.
Bowman, Rayleen V.
Fong, Kwun M.
MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression
title MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression
title_full MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression
title_fullStr MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression
title_full_unstemmed MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression
title_short MS4A1 Dysregulation in Asbestos-Related Lung Squamous Cell Carcinoma Is Due to CD20 Stromal Lymphocyte Expression
title_sort ms4a1 dysregulation in asbestos-related lung squamous cell carcinoma is due to cd20 stromal lymphocyte expression
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3325913/
https://www.ncbi.nlm.nih.gov/pubmed/22514692
http://dx.doi.org/10.1371/journal.pone.0034943
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