Experimental Models of Acute and Chronic Liver Failure in Nude Mice to Study Hepatocyte Transplantation

Author:

Gandillet Arnaud1,Vidal Isabelle12,Alexandre Eliane1,Audet Maxime12,Chenard-Neu Marie-Pierre3,Stutzmann Jeanne4,Heyd Bruno5,Jaeck Daniel12,Richert Lysiane16

Affiliation:

1. Laboratoire de Chirurgie Expérimentale, Fondation Transplantation, 67200 Strasbourg, France

2. Centre de Chirurgie Viscérale et de Transplantation, Hôpital de Hautepierre, 67098 Strasbourg, France

3. Service d'Anatomo-Pathologie, Hôpital de Hautepierre, 67098 Strasbourg, France

4. INSERM U381, 67200 Strasbourg, France

5. Service de Chirurgie Digestive et Vasculaire, Hôpital Jean Minjoz, 25000, Besançon, France

6. Laboratoire de Biologie Cellulaire, Faculté de Médecine et de Pharmacie, 25030 Besançon, France

Abstract

Although hepatocyte transplantation is a promising therapy for acute liver failure in human, there is still a lack of animal models suffering from hepatic injury in which the benefits of hepatocyte transplantation could be evaluated solely, without the bias caused by immunosuppression. As a consequence, the aim of the study was first to develop reproducible models of partial hepatectomy and of thioacetamide (TA)- or Jo2-induced acute liver failure in nude mice. Chronic liver disease was also investigated by repeated injections of sublethal doses of thioacetamide. Survival rates, routine histologic observations, alanin aminotransferase sera content, Ki67, and caspase 3 immunodetection were investigated both after 40% partial hepatectomy and after toxic-induced damages. Liver injuries were more severe and/or precocious in nude mice than in Balb/c mice for a given treatment with a maximum of acute injury obtained 24 h after single toxic injection, and were found to be transitory and reversible within 10 days. Toxics induced apoptosis followed by necrosis, confirming recent published data. Onset of fibrosis leading to reproducible chronic cirrhosis in nude mice correlated with increasing number of Ki67-positive cells, indicating that high levels of cell proliferation occurred. Chronic cirrhosis progressively reversed to fibrosis when the treatment ceased. Preliminary results demonstrated that engrafted xenogeneic hepatocytes could be detected in the host liver by anti-MHC class I immunohistochemistry. Fractions enriched in 2n or 4n hepatocytes by cell sorting using a flow cytometer were equivalent to the unpurified fraction in terms of engraftment in control nude mice or in nude mice subjected to PH. However, in mice suffering from liver injury 24 h after Jo2 or TA treatment, the engraftment of 2n hepatocytes was about twice that of an unpurified hepatocyte population or of a population enriched in 4n hepatocytes.

Publisher

SAGE Publications

Subject

Transplantation,Cell Biology,Biomedical Engineering

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