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Activin A, exendin-4, and glucose stimulate differentiation of human pancreatic ductal cells.

J Endocrinol · 2013

Last updated 2026-05-28

Scientists tested whether two substances, activin A and exendin-4 (a drug similar to GLP-1), could help human pancreatic duct cells turn into insulin-producing cells for diabetes treatment. In lab and mouse studies, combining these substances with high blood sugar levels helped the cells produce insulin and improve blood sugar control. When these treated cells were transplanted into diabetic mice, their blood sugar levels returned to normal.

AI summary of the abstract below.

JournalJ Endocrinol, 2013
Citations20
Relative citation ratio0.51
NIH percentile30
Molecules
Conditions studied Type 2 Diabetes

Abstract

Islet transplantation is one treatment option for diabetes mellitus. However, novel sources of pancreatic islets or insulin-producing cells are required because the amount of donor tissue available is severely limited. Pancreatic ductal cells are an alternative source of β-cells because they have the potential to differentiate into insulin-producing cells. We investigated whether treatment of human pancreatic ductal cells with activin A (ActA) and exendin-4 (EX-4) stimulated transdifferentiation of the cells, both in vitro and in vivo. We treated human pancreatic ductal cells with ActA and EX-4 in high-glucose media to induce differentiation into insulin-producing cells and transplanted the cells into streptozotocin-induced diabetic nude mice. Co-treatment of mice with ActA and EX-4 promoted cell proliferation, induced expression of pancreatic β-cell-specific markers, and caused glucose-induced insulin secretion compared with the ActA or EX-4 mono-treatment groups respectively. When pancreatic ductal cells treated with ActA and EX-4 in high-glucose media were transplanted into diabetic nude mice, their blood glucose levels normalized and insulin was detected in the graft. These findings suggest that pancreatic ductal cells have a potential to replace pancreatic islets for the treatment of diabetes mellitus when the ductal cells are co-treated with ActA, EX-4, and glucose to promote their differentiation into functional insulin-producing cells.

Verbatim abstract via PubMed 23503774 ↗