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GFAP promoter driven transgenic expression of PDGFB in the mouse brain leads to glioblastoma in a Trp53 null background

Glioblastomas are the most common and malignant astrocytic brain tumors in human adults. The tumor suppressor gene TP53 is commonly mutated and/or lost in astrocytic brain tumors and the TP53 alterations are often found in combination with excessive growth factor signaling via PDGF/PDGFRα. Here, we...

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Bibliographic Details
Published in:Glia 2009-08, Vol.57 (11), p.1143-1153
Main Authors: Hede, Sanna-Maria, Hansson, Inga, Afink, Gijs B., Eriksson, Anna, Nazarenko, Inga, Andrae, Johanna, Genove, Guillem, Westermark, Bengt, Nistér, Monica
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Language:English
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Summary:Glioblastomas are the most common and malignant astrocytic brain tumors in human adults. The tumor suppressor gene TP53 is commonly mutated and/or lost in astrocytic brain tumors and the TP53 alterations are often found in combination with excessive growth factor signaling via PDGF/PDGFRα. Here, we have generated transgenic mice over‐expressing human PDGFB in brain, under control of the human GFAP promoter. These mice showed no phenotype, but on a Trp53 null background a majority of them developed brain tumors. This occurred at 2–6 months of age and tumors displayed human glioblastoma‐like features with integrated development of Pdgfrα+ tumor cells and Pdgfrβ+/Nestin+ vasculature. The transgene was expressed in subependymal astrocytic cells, in glia limitans, and in astrocytes throughout the brain substance, and subsequently, microscopic tumor lesions were initiated equally in all these areas. With tumor size, there was an increase in Nestin positivity and variability in lineage markers. These results indicate an unexpected plasticity of all astrocytic cells in the adult brain, not only of SVZ cells. The results also indicate a contribution of widely distributed Pdgfrα+ precursor cells in the tumorigenic process. © 2008 Wiley‐Liss, Inc.
ISSN:0894-1491
1098-1136
1098-1136
DOI:10.1002/glia.20837