Selective Evolution of Stromal Mesenchyme with p53 Loss in Response to Epithelial Tumorigenesis

Our understanding of cancer has largely come from the analysis of aberrations within the tumor cell population. Yet it is increasingly clear that the tumor microenvironment can significantly influence tumorigenesis. For example, the mesenchyme can support the growth of tumorigenic epithelium. Howeve...

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Bibliographic Details
Published in:Cell 2005-12, Vol.123 (6), p.1001-1011
Main Authors: Hill, Reginald, Song, Yurong, Cardiff, Robert D., Van Dyke, Terry
Format: Article
Language:English
Subjects:
Actins - analysis
Adenocarcinoma - genetics
Adenocarcinoma - metabolism
Adenocarcinoma - pathology
Animals
Antigens, Polyomavirus Transforming - genetics
Cell Proliferation
Connective Tissue - pathology
Disease Models, Animal
Epithelial Cells - metabolism
Epithelial Cells - pathology
Fibroblasts - metabolism
Fibroblasts - pathology
Gene Deletion
Genotype
Keratin-8
Keratins - analysis
Loss of Heterozygosity - genetics
Male
Mice
Mice, Knockout
Mice, Transgenic
Models, Biological
Mutation - genetics
Paracrine Communication
Prostate - metabolism
Prostate - pathology
Prostatic Neoplasms - genetics
Prostatic Neoplasms - metabolism
Prostatic Neoplasms - pathology
Retinoblastoma Protein - metabolism
S100 Calcium-Binding Protein A4
S100 Proteins - analysis
Stromal Cells - metabolism
Stromal Cells - pathology
Tumor Suppressor Protein p53 - genetics
Tumor Suppressor Protein p53 - metabolism
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Summary:Our understanding of cancer has largely come from the analysis of aberrations within the tumor cell population. Yet it is increasingly clear that the tumor microenvironment can significantly influence tumorigenesis. For example, the mesenchyme can support the growth of tumorigenic epithelium. However, whether fibroblasts are subject to genetic/epigenetic changes as a result of selective pressures conferred by oncogenic stress in the epithelium has not been experimentally assessed. Recent analyses of some human carcinomas have shown tumor-suppressor gene mutations within the stroma, suggesting that the interplay among multiple cell types can select for aberrations nonautonomously during tumor progression. We demonstrate that this indeed occurs in a mouse model of prostate cancer where epithelial cell cycle disruption via cell-specific inhibition of pRb function induces a paracrine p53 response that suppresses fibroblast proliferation in associated stroma. This interaction imposes strong selective pressure yielding a highly proliferative mesenchyme that has undergone p53 loss.
ISSN:0092-8674
DOI:10.1016/j.cell.2005.09.030