Tumor Promotion in Liver of Mice with a Conditional Cx26 Knockout

doi:10.1093/toxsci/kfn043

ToxSci Advance Access originally published online on February 27, 2008
Toxicological Sciences 2008 103(2):260-267; doi:10.1093/toxsci/kfn043

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Tumor Promotion in Liver of Mice with a Conditional Cx26 Knockout

Philip Marx-Stoelting^*, Johanna Mahr^*, Thomas Knorpp, Sandra Schreiber^*, Markus F. Templin, Thomas Ott, Albrecht Buchmann^* and Michael Schwarz^*^,1

^* Institute of Pharmacology and Toxicology, Department of Toxicology, University of Tübingen, Wilhelmstr. 56, 72074 Tübingen, Germany NMI, Markwiesenstr. 55, 72770 Reutlingen, Germany IZKF/Central Unit for Transgenic Animals, Ottfried-Mueller-Str. 27, 72076 Tübingen, Germany

¹ To whom correspondence should be addressed at Institute for Pharmacology and Toxicology, Wilhelmstr. 56, 72074 Tübingen, Germany. Fax: +49-7071-29-2273. E-mail: michael.schwarz{at}uni-tuebingen.de.

Received January 21, 2008; accepted February 19, 2008

Abstract

Connexin (Cx) 26 and 32 are the major gap junction proteinsin liver. We recently demonstrated that Cx32 is essential forphenobarbital (PB)–mediated tumor promotion in mouse liver.To investigate whether Cx26 plays a similar role, an initiation-promotionexperiment was conducted using mice with a liver-specific knockoutof Cx26. Control and Cx26-deficient mice were injected a singledose of N-nitrosodiethylamine (DEN, 90 µg/g b.wt.) at6 weeks of age and groups of mice were subsequently kept ona PB (0.05%) containing or control diet for 35 weeks. At theend of the experiment, the carcinogenic response in the liverwas monitored. Mice from PB treatment groups showed stronglyincreased liver weights compared with mice treated with DENalone, which was mostly due to a much higher tumor burden. Thetumor response in PB-treated mice of both strains was quitesimilar, but the number of smaller tumors and of enzyme-alteredneoplastic lesions was somewhat larger in PB-treated Cx26 knockout(Cx26 KO) compared with wild-type mice, whereas the volume fractionof enzyme-altered lesions was slightly reduced in PB-treatedCx26-deficient mice. There was no significant difference intumor prevalence between Cx26 KO and wild-type mice. Altogetherour present data show that elimination of Cx26 has only minoreffects on chemically induced mouse hepatocarcinogenesis, instriking contrast to the effects seen in Cx32 KO mice.

Key Words: connexin; liver; phenobarbital; tumor promotion; β-catenin.

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