Islet-Like Structures Generated In Vitro from Adult Human Liver Stem Cells Revert Hyperglycemia in Diabetic SCID Mice

被引:0
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作者
Victor Navarro-Tableros
Chiara Gai
Yonathan Gomez
Sara Giunti
Chiara Pasquino
Maria Chiara Deregibus
Marta Tapparo
Adriana Pitino
Ciro Tetta
Maria Felice Brizzi
Camillo Ricordi
Giovanni Camussi
机构
[1] University of Turin,2i3T – Scarl.
[2] University of Turin,Molecular Biotechnology Center (MBC)
[3] Fondazione per la Ricerca Biomedica-ONLUS,Department of Medical Sciences
[4] Molecular Biotechnology and Health Sciences,Diabetes Research Institute
[5] MBC,undefined
[6] Unicyte AG,undefined
[7] University of Miami,undefined
来源
Stem Cell Reviews and Reports | 2019年 / 15卷
关键词
Pancreatic islets; Pancreatic β cells; Insulin-producing stem cells; Diabetes; Liver stem cells; 3D culture;
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学科分类号
摘要
A potential therapeutic strategy for diabetes is the transplantation of induced-insulin secreting cells. Based on the common embryonic origin of liver and pancreas, we studied the potential of adult human liver stem-like cells (HLSC) to generate in vitro insulin-producing 3D spheroid structures (HLSC-ILS). HLSC-ILS were generated by a one-step protocol based on charge dependent aggregation of HLSC induced by protamine. 3D aggregation promoted the spontaneous differentiation into cells expressing insulin and several key markers of pancreatic β cells. HLSC-ILS showed endocrine granules similar to those seen in human β cells. In static and dynamic in vitro conditions, such structures produced C-peptide after stimulation with high glucose. HLSC-ILS significantly reduced hyperglycemia and restored a normo-glycemic profile when implanted in streptozotocin-diabetic SCID mice. Diabetic mice expressed human C-peptide and very low or undetectable levels of murine C-peptide. Hyperglycemia and a diabetic profile were restored after HLSC-ISL explant. The gene expression profile of in vitro generated HLSC-ILS showed a differentiation from HLSC profile and an endocrine commitment with the enhanced expression of several markers of β cell differentiation. The comparative analysis of gene expression profiles after 2 and 4 weeks of in vivo implantation showed a further β-cell differentiation, with a genetic profile still immature but closer to that of human islets. In conclusion, protamine-induced spheroid aggregation of HLSC triggers a spontaneous differentiation to an endocrine phenotype. Although the in vitro differentiated HLSC-ILS were immature, they responded to high glucose with insulin secretion and in vivo reversed hyperglycemia in diabetic SCID mice.
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页码:93 / 111
页数:18
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