Literature DB >> 21822615

Phenotype of single hepatocytes expressing an activated version of β-catenin in liver of transgenic mice.

Sandra Schreiber1, Benjamin Rignall, Albert Braeuning, Philip Marx-Stoelting, Thomas Ott, Albrecht Buchmann, Seddik Hammad, Jan G Hengstler, Michael Schwarz, Christoph Köhle.   

Abstract

The gene CTNNB1 encoding β-catenin is mutated in about 30% of hepatocellular carcinoma, generally often combined with other genetic alterations. In transgenic mice, it has been shown that activation of β-catenin in more than 70% of all hepatocytes causes immediate proliferation leading to hepatomegaly. In this study we established a novel mouse model where β-catenin is activated only in individual, dispersed hepatocytes. Hepatocyte-specific expression of activated point-mutated β-catenin (human β-catenin(S33Y)) was established using the Cre/loxP system. Expression of several downstream targets of β-catenin signaling such as glutamine synthetase and several cytochrome P450 isoforms was confirmed by immunostaining. Only a minor portion of hepatocytes expressed the β-catenin(S33Y) transgene, which were mainly positioned as dispersed individual cells within the normal liver parenchyma. The hepatocytes with activated β-catenin did not show increased proliferation and the mice did not develop hepatomegaly. In conclusion, activated β-catenin in single hepatocytes induces a gene expression pattern in hepatocytes which is similar to that of Ctnnb1-mutated mouse liver tumors, but is apparently not sufficient to induce increased cell proliferation. Therefore, onset of proliferation seems to require concomitant activation of β-catenin in clusters of hepatocytes, suggesting a role of cell-cell communication in this process.

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Year:  2011        PMID: 21822615     DOI: 10.1007/s10735-011-9342-6

Source DB:  PubMed          Journal:  J Mol Histol        ISSN: 1567-2379            Impact factor:   2.611


  33 in total

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3.  Tumor formation in liver of conditional β-catenin-deficient mice exposed to a diethylnitrosamine/phenobarbital tumor promotion regimen.

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4.  Mutation of beta-catenin is an early event in chemically induced mouse hepatocellular carcinogenesis.

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4.  Activating CAR and β-catenin induces uncontrolled liver growth and tumorigenesis.

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5.  Quantification of three-dimensional structures in liver tissue: bile canalicular and sinusoidal networks.

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6.  Protocols for staining of bile canalicular and sinusoidal networks of human, mouse and pig livers, three-dimensional reconstruction and quantification of tissue microarchitecture by image processing and analysis.

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Review 7.  β-catenin signaling, the constitutive androstane receptor and their mutual interactions.

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  7 in total

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