Human Liver Cells Expressing Albumin and Mesenchymal Characteristics Give Rise to Insulin-Producing Cells

Author:

Meivar-Levy Irit1,Sapir Tamar2ORCID,Berneman Dana13,Weissbach Tal4,Polak-Charcon Sylvie5,Ravassard Philippe6,Tzakis Andreas G.7ORCID,Mor Eytan8,Ricordi Camillo2,Ferber Sarah13

Affiliation:

1. Sheba Regenerative Medicine, Stem cells and Tissue engineering Center, Sheba Medical Center, Tel-Hashomer 52621, Israel

2. Diabetes Research Institute, University of Miami Leonard M. Miller School of Medicine, 1450 NW 10th Avenue, Miami, FL 33136, USA

3. Department of Human Genetics and Molecular Medicine, Sackler School of Medicine, Tel-Aviv University, 69978 Tel-Aviv, Israel

4. Obstetrics and Gynecology Department, Sapir Medical Ctrter 44281 Kfar Saba, Israel

5. The Institute for Pathology, Sheba Medical Center, 52621 Tel-Hashomer, Israel

6. Biotechnology and Biotherapy Group, Centre de Recherche, Institut du Cerveau et de la Moelle CNRS UMR7225, INSERM UMRS795, Université Pierre et Marie Curie, 75005 Paris, France

7. The Miami Transplant Institute, University of Miami Leonard M. Miller School of Medicine, 1450 NW 10th Avenue, Miami, FL 33136, USA

8. Rabin Medical Center, Beilinson Campus, 49100 Petah-Tiqva, Israel

Abstract

Activation of the pancreatic lineage in the liver has been suggested as a potential autologous cell replacement therapy for diabetic patients. Transcription factors-induced liver-to-pancreas reprogramming has been demonstrated in numerous species bothin vivoandin vitro. However, human-derived liver cells capable of acquiring the alternate pancreatic repertoire have never been characterized. It is yet unknown whether hepatic-like stem cells or rather adult liver cells give rise to insulin-producing cells. Using anin vitroexperimental system, we demonstrate that proliferating adherent human liver cells acquire mesenchymal-like characteristics and a considerable level of cellular plasticity. However, using a lineage-tracing approach, we demonstrate that insulin-producing cells are primarily generated in cells enriched for adult hepatic markers that coexpress both albumin and mesenchymal markers. Taken together, our data suggest that adult human hepatic tissue retains a substantial level of developmental plasticity, which could be exploited in regenerative medicine approaches.

Funder

Juvenile Diabetes Research Foundation International

Publisher

Hindawi Limited

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