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Publication : Hepatic tissue environment in NEMO-deficient mice critically regulates positive selection of donor cells after hepatocyte transplantation.

First Author  Kaldenbach M Year  2014
Journal  PLoS One Volume  9
Issue  6 Pages  e100786
PubMed ID  24979756 Mgi Jnum  J:216812
Mgi Id  MGI:5609727 Doi  10.1371/journal.pone.0100786
Citation  Kaldenbach M, et al. (2014) Hepatic tissue environment in NEMO-deficient mice critically regulates positive selection of donor cells after hepatocyte transplantation. PLoS One 9(6):e100786
abstractText  BACKGROUND: Hepatocyte transplantation (HT) is a promising alternative treatment strategy for end-stage liver diseases compared with orthotopic liver transplantation. A limitation for this approach is the low engraftment of donor cells. The deletion of the I-kappa B kinase-regulatory subunit IKKgamma/NEMO in hepatocytes prevents nuclear factor (NF)-kB activation and triggers spontaneous liver apoptosis, chronic hepatitis and the development of liver fibrosis and hepatocellular carcinoma. We hypothesized that NEMODeltahepa mice may therefore serve as an experimental model to study HT. METHODS: Pre-conditioned NEMODeltahepa mice were transplanted with donor-hepatocytes from wildtype (WT) and mice deficient for the pro-apoptotic mediator Caspase-8 (Casp8Deltahepa). RESULTS: Transplantation of isolated WT-hepatocytes into pre-conditioned NEMODeltahepa mice resulted in a 6-7 fold increase of donor cells 12 weeks after HT, while WT-recipients showed no liver repopulation. The use of apoptosis-resistant Casp8Deltahepa-derived donor cells further enhanced the selection 3-fold after 12-weeks and up to 10-fold increase after 52 weeks compared with WT donors. While analysis of NEMODeltahepa mice revealed strong liver injury, HT-recipient NEMODeltahepa mice showed improved liver morphology and decrease in serum transaminases. Concomitant with these findings, the histological examination elicited an improved liver tissue architecture associated with significantly lower levels of apoptosis, decreased proliferation and a lesser amount of liver fibrogenesis. Altogether, our data clearly support the therapeutic benefit of the HT procedure into NEMODeltahepa mice. CONCLUSION: This study demonstrates the feasibility of the NEMODeltahepa mouse as an in vivo tool to study liver repopulation after HT. The improvement of the characteristic phenotype of chronic liver injury in NEMODeltahepa mice after HT suggests the therapeutic potential of HT in liver diseases with a chronic inflammatory phenotype and opens a new door for the applicability of this technique to combat liver disease in the human clinic.
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