Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver

Resection of hepatocellular carcinoma (HCC) tumors by partial hepatectomy (PHx) is associated with promoting hepatocarcinogenesis. We have previously reported that PHx promotes hepatocarcinogenesis in the Mdr2-knockout (Mdr2-KO) mouse, a model for inflammation-mediated HCC. Now, to explore the molec...

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Autores principales: Ella, Ezra, Heim, Denise, Stoyanov, Evgeniy, Harari-Steinfeld, Rona, Steinfeld, Israel, Pappo, Orit, Perlman, Temima Schnitzer, Nachmansson, Natalie, Rivkin, Ludmila, Olam, Devorah, Abramovitch, Rinat, Wege, Henning, Galun, Eithan, Goldenberg, Daniel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4279375/
https://www.ncbi.nlm.nih.gov/pubmed/25401338
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author Ella, Ezra
Heim, Denise
Stoyanov, Evgeniy
Harari-Steinfeld, Rona
Steinfeld, Israel
Pappo, Orit
Perlman, Temima Schnitzer
Nachmansson, Natalie
Rivkin, Ludmila
Olam, Devorah
Abramovitch, Rinat
Wege, Henning
Galun, Eithan
Goldenberg, Daniel
author_facet Ella, Ezra
Heim, Denise
Stoyanov, Evgeniy
Harari-Steinfeld, Rona
Steinfeld, Israel
Pappo, Orit
Perlman, Temima Schnitzer
Nachmansson, Natalie
Rivkin, Ludmila
Olam, Devorah
Abramovitch, Rinat
Wege, Henning
Galun, Eithan
Goldenberg, Daniel
author_sort Ella, Ezra
collection PubMed
description Resection of hepatocellular carcinoma (HCC) tumors by partial hepatectomy (PHx) is associated with promoting hepatocarcinogenesis. We have previously reported that PHx promotes hepatocarcinogenesis in the Mdr2-knockout (Mdr2-KO) mouse, a model for inflammation-mediated HCC. Now, to explore the molecular mechanisms underlying the tumor-promoting effect of PHx, we compared genomic and transcriptomic profiles of HCC tumors developing in the Mdr2-KO mice either spontaneously or following PHx. PHx accelerated HCC development in these mice by four months. PHx-induced tumors had major chromosomal aberrations: all were amplifications affecting multiple chromosomes. Most of these amplifications were located near the acrocentric centromeres of murine chromosomes. Four different chromosomal regions were amplified each in at least three tumors. The human orthologs of these common amplified regions are known to be amplified in HCC. All tumors of untreated mice had chromosomal aberrations, including both deletions and amplifications. Amplifications in spontaneous tumors affected fewer chromosomes and were not located preferentially at the chromosomal edges. Comparison of gene expression profiles revealed a significantly enriched expression of oncogenes, chromosomal instability markers and E2F1 targets in the post-PHx compared to spontaneous tumors. Both tumor groups shared the same frequent amplification at chromosome 18. Here, we revealed that one of the regulatory genes encoded by this amplified region, Crem, was over-expressed in the nuclei of murine and human HCC cells in vivo, and that it stimulated proliferation of human HCC cells in vitro. Our results demonstrate that PHx of a chronically inflamed liver directed tumor development to a discrete pathway characterized by amplification of specific chromosomal regions and expression of specific tumor-promoting genes. Crem is a new candidate HCC oncogene frequently amplified in this model and frequently over-expressed in human HCC.
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spelling pubmed-42793752015-01-06 Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver Ella, Ezra Heim, Denise Stoyanov, Evgeniy Harari-Steinfeld, Rona Steinfeld, Israel Pappo, Orit Perlman, Temima Schnitzer Nachmansson, Natalie Rivkin, Ludmila Olam, Devorah Abramovitch, Rinat Wege, Henning Galun, Eithan Goldenberg, Daniel Oncotarget Research Paper Resection of hepatocellular carcinoma (HCC) tumors by partial hepatectomy (PHx) is associated with promoting hepatocarcinogenesis. We have previously reported that PHx promotes hepatocarcinogenesis in the Mdr2-knockout (Mdr2-KO) mouse, a model for inflammation-mediated HCC. Now, to explore the molecular mechanisms underlying the tumor-promoting effect of PHx, we compared genomic and transcriptomic profiles of HCC tumors developing in the Mdr2-KO mice either spontaneously or following PHx. PHx accelerated HCC development in these mice by four months. PHx-induced tumors had major chromosomal aberrations: all were amplifications affecting multiple chromosomes. Most of these amplifications were located near the acrocentric centromeres of murine chromosomes. Four different chromosomal regions were amplified each in at least three tumors. The human orthologs of these common amplified regions are known to be amplified in HCC. All tumors of untreated mice had chromosomal aberrations, including both deletions and amplifications. Amplifications in spontaneous tumors affected fewer chromosomes and were not located preferentially at the chromosomal edges. Comparison of gene expression profiles revealed a significantly enriched expression of oncogenes, chromosomal instability markers and E2F1 targets in the post-PHx compared to spontaneous tumors. Both tumor groups shared the same frequent amplification at chromosome 18. Here, we revealed that one of the regulatory genes encoded by this amplified region, Crem, was over-expressed in the nuclei of murine and human HCC cells in vivo, and that it stimulated proliferation of human HCC cells in vitro. Our results demonstrate that PHx of a chronically inflamed liver directed tumor development to a discrete pathway characterized by amplification of specific chromosomal regions and expression of specific tumor-promoting genes. Crem is a new candidate HCC oncogene frequently amplified in this model and frequently over-expressed in human HCC. Impact Journals LLC 2014-09-25 /pmc/articles/PMC4279375/ /pubmed/25401338 Text en Copyright: © 2014 Ella et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Ella, Ezra
Heim, Denise
Stoyanov, Evgeniy
Harari-Steinfeld, Rona
Steinfeld, Israel
Pappo, Orit
Perlman, Temima Schnitzer
Nachmansson, Natalie
Rivkin, Ludmila
Olam, Devorah
Abramovitch, Rinat
Wege, Henning
Galun, Eithan
Goldenberg, Daniel
Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
title Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
title_full Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
title_fullStr Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
title_full_unstemmed Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
title_short Specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
title_sort specific genomic and transcriptomic aberrations in tumors induced by partial hepatectomy of a chronically inflamed murine liver
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4279375/
https://www.ncbi.nlm.nih.gov/pubmed/25401338
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