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Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer

BACKGROUND: The expression of carcino-embryonic antigen by colorectal cancer is an example of oncogenic activation of embryonic gene expression. Hypothesizing that oncogenesis-recapitulating-ontogenesis may represent a broad programmatic commitment, we compared gene expression patterns of human colo...

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Autores principales: Kaiser, Sergio, Park, Young-Kyu, Franklin, Jeffrey L, Halberg, Richard B, Yu, Ming, Jessen, Walter J, Freudenberg, Johannes, Chen, Xiaodi, Haigis, Kevin, Jegga, Anil G, Kong, Sue, Sakthivel, Bhuvaneswari, Xu, Huan, Reichling, Timothy, Azhar, Mohammad, Boivin, Gregory P, Roberts, Reade B, Bissahoyo, Anika C, Gonzales, Fausto, Bloom, Greg C, Eschrich, Steven, Carter, Scott L, Aronow, Jeremy E, Kleimeyer, John, Kleimeyer, Michael, Ramaswamy, Vivek, Settle, Stephen H, Boone, Braden, Levy, Shawn, Graff, Jonathan M, Doetschman, Thomas, Groden, Joanna, Dove, William F, Threadgill, David W, Yeatman, Timothy J, Coffey, Robert J, Aronow, Bruce J
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2323222/
https://www.ncbi.nlm.nih.gov/pubmed/17615082
http://dx.doi.org/10.1186/gb-2007-8-7-r131
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author Kaiser, Sergio
Park, Young-Kyu
Franklin, Jeffrey L
Halberg, Richard B
Yu, Ming
Jessen, Walter J
Freudenberg, Johannes
Chen, Xiaodi
Haigis, Kevin
Jegga, Anil G
Kong, Sue
Sakthivel, Bhuvaneswari
Xu, Huan
Reichling, Timothy
Azhar, Mohammad
Boivin, Gregory P
Roberts, Reade B
Bissahoyo, Anika C
Gonzales, Fausto
Bloom, Greg C
Eschrich, Steven
Carter, Scott L
Aronow, Jeremy E
Kleimeyer, John
Kleimeyer, Michael
Ramaswamy, Vivek
Settle, Stephen H
Boone, Braden
Levy, Shawn
Graff, Jonathan M
Doetschman, Thomas
Groden, Joanna
Dove, William F
Threadgill, David W
Yeatman, Timothy J
Coffey, Robert J
Aronow, Bruce J
author_facet Kaiser, Sergio
Park, Young-Kyu
Franklin, Jeffrey L
Halberg, Richard B
Yu, Ming
Jessen, Walter J
Freudenberg, Johannes
Chen, Xiaodi
Haigis, Kevin
Jegga, Anil G
Kong, Sue
Sakthivel, Bhuvaneswari
Xu, Huan
Reichling, Timothy
Azhar, Mohammad
Boivin, Gregory P
Roberts, Reade B
Bissahoyo, Anika C
Gonzales, Fausto
Bloom, Greg C
Eschrich, Steven
Carter, Scott L
Aronow, Jeremy E
Kleimeyer, John
Kleimeyer, Michael
Ramaswamy, Vivek
Settle, Stephen H
Boone, Braden
Levy, Shawn
Graff, Jonathan M
Doetschman, Thomas
Groden, Joanna
Dove, William F
Threadgill, David W
Yeatman, Timothy J
Coffey, Robert J
Aronow, Bruce J
author_sort Kaiser, Sergio
collection PubMed
description BACKGROUND: The expression of carcino-embryonic antigen by colorectal cancer is an example of oncogenic activation of embryonic gene expression. Hypothesizing that oncogenesis-recapitulating-ontogenesis may represent a broad programmatic commitment, we compared gene expression patterns of human colorectal cancers (CRCs) and mouse colon tumor models to those of mouse colon development embryonic days 13.5-18.5. RESULTS: We report here that 39 colon tumors from four independent mouse models and 100 human CRCs encompassing all clinical stages shared a striking recapitulation of embryonic colon gene expression. Compared to normal adult colon, all mouse and human tumors over-expressed a large cluster of genes highly enriched for functional association to the control of cell cycle progression, proliferation, and migration, including those encoding MYC, AKT2, PLK1 and SPARC. Mouse tumors positive for nuclear β-catenin shifted the shared embryonic pattern to that of early development. Human and mouse tumors differed from normal embryonic colon by their loss of expression modules enriched for tumor suppressors (EDNRB, HSPE, KIT and LSP1). Human CRC adenocarcinomas lost an additional suppressor module (IGFBP4, MAP4K1, PDGFRA, STAB1 and WNT4). Many human tumor samples also gained expression of a coordinately regulated module associated with advanced malignancy (ABCC1, FOXO3A, LIF, PIK3R1, PRNP, TNC, TIMP3 and VEGF). CONCLUSION: Cross-species, developmental, and multi-model gene expression patterning comparisons provide an integrated and versatile framework for definition of transcriptional programs associated with oncogenesis. This approach also provides a general method for identifying pattern-specific biomarkers and therapeutic targets. This delineation and categorization of developmental and non-developmental activator and suppressor gene modules can thus facilitate the formulation of sophisticated hypotheses to evaluate potential synergistic effects of targeting within- and between-modules for next-generation combinatorial therapeutics and improved mouse models.
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spelling pubmed-23232222008-04-19 Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer Kaiser, Sergio Park, Young-Kyu Franklin, Jeffrey L Halberg, Richard B Yu, Ming Jessen, Walter J Freudenberg, Johannes Chen, Xiaodi Haigis, Kevin Jegga, Anil G Kong, Sue Sakthivel, Bhuvaneswari Xu, Huan Reichling, Timothy Azhar, Mohammad Boivin, Gregory P Roberts, Reade B Bissahoyo, Anika C Gonzales, Fausto Bloom, Greg C Eschrich, Steven Carter, Scott L Aronow, Jeremy E Kleimeyer, John Kleimeyer, Michael Ramaswamy, Vivek Settle, Stephen H Boone, Braden Levy, Shawn Graff, Jonathan M Doetschman, Thomas Groden, Joanna Dove, William F Threadgill, David W Yeatman, Timothy J Coffey, Robert J Aronow, Bruce J Genome Biol Research BACKGROUND: The expression of carcino-embryonic antigen by colorectal cancer is an example of oncogenic activation of embryonic gene expression. Hypothesizing that oncogenesis-recapitulating-ontogenesis may represent a broad programmatic commitment, we compared gene expression patterns of human colorectal cancers (CRCs) and mouse colon tumor models to those of mouse colon development embryonic days 13.5-18.5. RESULTS: We report here that 39 colon tumors from four independent mouse models and 100 human CRCs encompassing all clinical stages shared a striking recapitulation of embryonic colon gene expression. Compared to normal adult colon, all mouse and human tumors over-expressed a large cluster of genes highly enriched for functional association to the control of cell cycle progression, proliferation, and migration, including those encoding MYC, AKT2, PLK1 and SPARC. Mouse tumors positive for nuclear β-catenin shifted the shared embryonic pattern to that of early development. Human and mouse tumors differed from normal embryonic colon by their loss of expression modules enriched for tumor suppressors (EDNRB, HSPE, KIT and LSP1). Human CRC adenocarcinomas lost an additional suppressor module (IGFBP4, MAP4K1, PDGFRA, STAB1 and WNT4). Many human tumor samples also gained expression of a coordinately regulated module associated with advanced malignancy (ABCC1, FOXO3A, LIF, PIK3R1, PRNP, TNC, TIMP3 and VEGF). CONCLUSION: Cross-species, developmental, and multi-model gene expression patterning comparisons provide an integrated and versatile framework for definition of transcriptional programs associated with oncogenesis. This approach also provides a general method for identifying pattern-specific biomarkers and therapeutic targets. This delineation and categorization of developmental and non-developmental activator and suppressor gene modules can thus facilitate the formulation of sophisticated hypotheses to evaluate potential synergistic effects of targeting within- and between-modules for next-generation combinatorial therapeutics and improved mouse models. BioMed Central 2007 2007-07-05 /pmc/articles/PMC2323222/ /pubmed/17615082 http://dx.doi.org/10.1186/gb-2007-8-7-r131 Text en Copyright © 2007 Kaiser et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Kaiser, Sergio
Park, Young-Kyu
Franklin, Jeffrey L
Halberg, Richard B
Yu, Ming
Jessen, Walter J
Freudenberg, Johannes
Chen, Xiaodi
Haigis, Kevin
Jegga, Anil G
Kong, Sue
Sakthivel, Bhuvaneswari
Xu, Huan
Reichling, Timothy
Azhar, Mohammad
Boivin, Gregory P
Roberts, Reade B
Bissahoyo, Anika C
Gonzales, Fausto
Bloom, Greg C
Eschrich, Steven
Carter, Scott L
Aronow, Jeremy E
Kleimeyer, John
Kleimeyer, Michael
Ramaswamy, Vivek
Settle, Stephen H
Boone, Braden
Levy, Shawn
Graff, Jonathan M
Doetschman, Thomas
Groden, Joanna
Dove, William F
Threadgill, David W
Yeatman, Timothy J
Coffey, Robert J
Aronow, Bruce J
Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
title Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
title_full Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
title_fullStr Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
title_full_unstemmed Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
title_short Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
title_sort transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2323222/
https://www.ncbi.nlm.nih.gov/pubmed/17615082
http://dx.doi.org/10.1186/gb-2007-8-7-r131
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