Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients

BACKGROUND: Genetic and epigenetic alterations in colorectal cancer are numerous. However, it is difficult to judge whether such changes are primary or secondary to the appearance and progression of tumors. Therefore, the aim of the present study was to identify altered DNA regions with significant...

Descripción completa

Detalles Bibliográficos
Autores principales: Lagerstedt, Kristina K., Kristiansson, Erik, Lönnroth, Christina, Andersson, Marianne, Iresjö, Britt-Marie, Gustafsson, Annika, Hansson, Elisabeth, Kressner, Ulf, Nordgren, Svante, Enlund, Fredrik, Lundholm, Kent
Formato: Texto
Lenguaje:English
Publicado: Libertas Academica 2010
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2867635/
https://www.ncbi.nlm.nih.gov/pubmed/20467480
_version_ 1782180990107516928
author Lagerstedt, Kristina K.
Kristiansson, Erik
Lönnroth, Christina
Andersson, Marianne
Iresjö, Britt-Marie
Gustafsson, Annika
Hansson, Elisabeth
Kressner, Ulf
Nordgren, Svante
Enlund, Fredrik
Lundholm, Kent
author_facet Lagerstedt, Kristina K.
Kristiansson, Erik
Lönnroth, Christina
Andersson, Marianne
Iresjö, Britt-Marie
Gustafsson, Annika
Hansson, Elisabeth
Kressner, Ulf
Nordgren, Svante
Enlund, Fredrik
Lundholm, Kent
author_sort Lagerstedt, Kristina K.
collection PubMed
description BACKGROUND: Genetic and epigenetic alterations in colorectal cancer are numerous. However, it is difficult to judge whether such changes are primary or secondary to the appearance and progression of tumors. Therefore, the aim of the present study was to identify altered DNA regions with significant covariation to transcription alterations along colon cancer progression. METHODS: Tumor and normal colon tissue were obtained at primary operations from 24 patients selected by chance. DNA, RNA and microRNAs were extracted from the same biopsy material in all individuals and analyzed by oligo-nucleotide array-based comparative genomic hybridization (CGH), mRNA- and microRNA oligo-arrays. Statistical analyses were performed to assess statistical interactions (correlations, co-variations) between DNA copy number changes and significant alterations in gene and microRNA expression using appropriate parametric and non-parametric statistics. RESULTS: Main DNA alterations were located on chromosome 7, 8, 13 and 20. Tumor DNA copy number gain increased with tumor progression, significantly related to increased gene expression. Copy number loss was not observed in Dukes A tumors. There was no significant relationship between expressed genes and tumor progression across Dukes A–D tumors; and no relationship between tumor stage and the number of microRNAs with significantly altered expression. Interaction analyses identified overall 41 genes, which discriminated early Dukes A plus B tumors from late Dukes C plus D tumor; 28 of these genes remained with correlations between genomic and transcriptomic alterations in Dukes C plus D tumors and 17 in Dukes D. One microRNA (microR-663) showed interactions with DNA alterations in all Dukes A-D tumors. CONCLUSIONS: Our modeling confirms that colon cancer progression is related to genomic instability and altered gene expression. However, early invasive tumor growth seemed rather related to transcriptomic alterations, where changes in microRNA may be an early phenomenon, and less to DNA copy number changes.
format Text
id pubmed-2867635
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Libertas Academica
record_format MEDLINE/PubMed
spelling pubmed-28676352010-05-13 Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients Lagerstedt, Kristina K. Kristiansson, Erik Lönnroth, Christina Andersson, Marianne Iresjö, Britt-Marie Gustafsson, Annika Hansson, Elisabeth Kressner, Ulf Nordgren, Svante Enlund, Fredrik Lundholm, Kent Cancer Inform Original Research BACKGROUND: Genetic and epigenetic alterations in colorectal cancer are numerous. However, it is difficult to judge whether such changes are primary or secondary to the appearance and progression of tumors. Therefore, the aim of the present study was to identify altered DNA regions with significant covariation to transcription alterations along colon cancer progression. METHODS: Tumor and normal colon tissue were obtained at primary operations from 24 patients selected by chance. DNA, RNA and microRNAs were extracted from the same biopsy material in all individuals and analyzed by oligo-nucleotide array-based comparative genomic hybridization (CGH), mRNA- and microRNA oligo-arrays. Statistical analyses were performed to assess statistical interactions (correlations, co-variations) between DNA copy number changes and significant alterations in gene and microRNA expression using appropriate parametric and non-parametric statistics. RESULTS: Main DNA alterations were located on chromosome 7, 8, 13 and 20. Tumor DNA copy number gain increased with tumor progression, significantly related to increased gene expression. Copy number loss was not observed in Dukes A tumors. There was no significant relationship between expressed genes and tumor progression across Dukes A–D tumors; and no relationship between tumor stage and the number of microRNAs with significantly altered expression. Interaction analyses identified overall 41 genes, which discriminated early Dukes A plus B tumors from late Dukes C plus D tumor; 28 of these genes remained with correlations between genomic and transcriptomic alterations in Dukes C plus D tumors and 17 in Dukes D. One microRNA (microR-663) showed interactions with DNA alterations in all Dukes A-D tumors. CONCLUSIONS: Our modeling confirms that colon cancer progression is related to genomic instability and altered gene expression. However, early invasive tumor growth seemed rather related to transcriptomic alterations, where changes in microRNA may be an early phenomenon, and less to DNA copy number changes. Libertas Academica 2010-04-23 /pmc/articles/PMC2867635/ /pubmed/20467480 Text en © the author(s), publisher and licensee Libertas Academica Ltd. http://creativecommons.org/licenses/by/3.0 This article is an open-access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/).
spellingShingle Original Research
Lagerstedt, Kristina K.
Kristiansson, Erik
Lönnroth, Christina
Andersson, Marianne
Iresjö, Britt-Marie
Gustafsson, Annika
Hansson, Elisabeth
Kressner, Ulf
Nordgren, Svante
Enlund, Fredrik
Lundholm, Kent
Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients
title Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients
title_full Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients
title_fullStr Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients
title_full_unstemmed Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients
title_short Genes with Relevance for Early to Late Progression of Colon Carcinoma Based on Combined Genomic and Transcriptomic Information from the Same Patients
title_sort genes with relevance for early to late progression of colon carcinoma based on combined genomic and transcriptomic information from the same patients
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2867635/
https://www.ncbi.nlm.nih.gov/pubmed/20467480
work_keys_str_mv AT lagerstedtkristinak geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT kristianssonerik geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT lonnrothchristina geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT anderssonmarianne geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT iresjobrittmarie geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT gustafssonannika geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT hanssonelisabeth geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT kressnerulf geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT nordgrensvante geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT enlundfredrik geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients
AT lundholmkent geneswithrelevanceforearlytolateprogressionofcoloncarcinomabasedoncombinedgenomicandtranscriptomicinformationfromthesamepatients

Ejemplares similares