| Literature DB >> 32031745 |
Fanny Lebreton1, Kevin Bellofatto1, Charles H Wassmer1, Lisa Perez1, Vanessa Lavallard1, Géraldine Parnaud1, David Cottet-Dumoulin1, Julie Kerr-Conte2, François Pattou2, Domenico Bosco1, Véronique Othenin-Girard3, Begoña Martinez de Tejada3,4, Ekaterine Berishvili1,5.
Abstract
Hypoxia is a major cause of considerable islet loss during the early posttransplant period. Here, we investigate whether shielding islets with human amniotic epithelial cells (hAECs), which possess anti-inflammatory and regenerative properties, improves islet engraftment and survival. Shielded islets were generated on agarose microwells by mixing rat islets (RIs) or human islets (HI) and hAECs (100 hAECs/IEQ). Islet secretory function and viability were assessed after culture in hypoxia (1% O2 ) or normoxia (21% O2 ) in vitro. In vivo function was evaluated after transplant under the kidney capsule of diabetic immunodeficient mice. Graft morphology and vascularization were evaluated by immunohistochemistry. Both shielded RIs and HIs show higher viability and increased glucose-stimulated insulin secretion after exposure to hypoxia in vitro compared with control islets. Transplant of shielded islets results in considerably earlier normoglycemia and vascularization, an enhanced glucose tolerance, and a higher β cell mass. Our results show that hAECs have a clear cytoprotective effect against hypoxic damages in vitro. This strategy improves β cell mass engraftment and islet revascularization, leading to an improved capacity of islets to reverse hyperglycemia, and could be rapidly applicable in the clinical situation seeing that the modification to HIs are minor.Entities:
Keywords: basic (laboratory) research/science; diabetes: type 1; islet transplantation; islets of Langerhans; regenerative medicine; stem cells; tissue/organ engineering; translational research/science
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Year: 2020 PMID: 32031745 DOI: 10.1111/ajt.15812
Source DB: PubMed Journal: Am J Transplant ISSN: 1600-6135 Impact factor: 8.086