Human liver cells expressing albumin and mesenchymal characteristics give rise to insulin-producing cells.

表达白蛋白和间充质特征的人类肝细胞可分化为胰岛素分泌细胞

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作者:Meivar-Levy Irit, Sapir Tamar, Berneman Dana, Weissbach Tal, Polak-Charcon Sylvie, Ravassard Philippe, Tzakis Andreas G, Mor Eytan, Ricordi Camillo, Ferber Sarah
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 both in vivo and in 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 an in vitro experimental 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.

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