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The liver of tumor-bearing hosts manifests fetal phenotypes. We investigated the expression of differentiation markers on the liver in MMTV-neu (ErbB-2) transgenic mice, in the period from incipient neoangiogenesis to lung metastatization. We report AFP expression by hepatocytes in all lobular zones, CD34 cell arrest and subsequent hemopoiesis in periportal and mid-zone areas, oval-like cells (CD34+, CK19+, AFP+) and ductular reaction in portal tracts, portal CK19+ and GGT+ hepatoblast-like cells, and midzonal large dysplastic hepatocytes. We hypothesize that CD34 cells are recruited by the tumor from the marrow for angiogenic purposes and that their differentiation in the liver is influenced by altered liver microenvironment(s). AFP may act as a growth factor and biological response modifier for these cells and for the tumor. Dysplasia might be enhanced by metabolic stress. We conclude that the liver differentiation potential is lobularzone- dependent and that the risk for eventually developing a pre-malignant lesion is not negligible.

Stem Cell Recruitment and Liver De-Differentiation in MMTV-Neu (ErbB-2) Transgenic Mice

BUCETA SANDE DE FREITAS, MARIA ISABEL;FRACCHIOLLA, SIMONA;GRIFFINI, PATRIZIA;BERTONE, ROBERTA;SITAR, GIAMMARIA;BARNI, SERGIO;GERZELI, GIUSEPPE;
2003-01-01

Abstract

The liver of tumor-bearing hosts manifests fetal phenotypes. We investigated the expression of differentiation markers on the liver in MMTV-neu (ErbB-2) transgenic mice, in the period from incipient neoangiogenesis to lung metastatization. We report AFP expression by hepatocytes in all lobular zones, CD34 cell arrest and subsequent hemopoiesis in periportal and mid-zone areas, oval-like cells (CD34+, CK19+, AFP+) and ductular reaction in portal tracts, portal CK19+ and GGT+ hepatoblast-like cells, and midzonal large dysplastic hepatocytes. We hypothesize that CD34 cells are recruited by the tumor from the marrow for angiogenic purposes and that their differentiation in the liver is influenced by altered liver microenvironment(s). AFP may act as a growth factor and biological response modifier for these cells and for the tumor. Dysplasia might be enhanced by metabolic stress. We conclude that the liver differentiation potential is lobularzone- dependent and that the risk for eventually developing a pre-malignant lesion is not negligible.
2003
Cell & Developmental Biology contains resources in biochemistry, molecular biology, biophysics, physiology, and pharmacology that have a specific emphasis on cellular function in eukaryotic systems. Topics of particular importance include receptor biology and signal transduction, regulation of gene expression at the cellular level, developmental genetics, developmental biology and morphogenesis, and cell-environment interactions. Resources concentrated on molecular biochemistry and molecular regulation of gene expression, as well as microscopic or histological analysis of cell or tissue samples are excluded.
ANTICANCER RESEARCH
Esperti anonimi
Inglese
Internazionale
STAMPA
23
3783
3794
Tematica Ex SIR: Morfogenesi, cicli biologici e alterazioni patologiche in cellule, tessuti e organi dei Vertebrati (Classif. Ex SIR:Articoli su riviste ISI )
Liver; hemopoietic stem cells; oval cells; de-differentiation; large liver cell dysplasia; cytokeratins; α-fetoprotein
9
info:eu-repo/semantics/article
262
BUCETA SANDE DE FREITAS, MARIA ISABEL; Fracchiolla, Simona; Baronzio, G. F.; Griffini, Patrizia; Bertone, Roberta; Sitar, Giammaria; Barni, Sergio; Ge...espandi
1 Contributo su Rivista::1.1 Articolo in rivista
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1.1 Articolo in rivista
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11571/136921
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