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- GLP-1 receptor agonists synergize with DYRK1A inhibitors to potentiate functional human β cell regeneration.
GLP-1 receptor agonists synergize with DYRK1A inhibitors to potentiate functional human β cell regeneration.
Citation | “Glp-1 Receptor Agonists Synergize With Dyrk1A Inhibitors To Potentiate Functional Human Β Cell Regeneration.”. Science Translational Medicine. . |
Center | Albert Einstein College of Medicine |
Featured |
Featured
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Author | Courtney Ackeifi, Peng Wang, Esra Karakose, Jocelyn E Manning Fox, Bryan J González, Hongtao Liu, Jessica Wilson, Ethan Swartz, Cecilia Berrouet, Yansui Li, Kunal Kumar, Patrick E MacDonald, Roberto Sanchez, Bernard Thorens, Robert DeVita, Dirk Homann, Dieter Egli, Donald K Scott, Adolfo Garcia-Ocaña, Andrew F Stewart |
Abstract |
Glucagon-like peptide-1 receptor (GLP1R) agonists and dipeptidyl peptidase 4 inhibitors are widely prescribed diabetes drugs due to their ability to stimulate insulin secretion from remaining β cells and to reduce caloric intake. Unfortunately, they fail to increase human β cell proliferation. Small-molecule inhibitors of dual-specificity tyrosine-regulated kinase 1A (DYRK1A) are able to induce adult human β cell proliferation, but rates are modest (~2%), and their specificity to β cells is limited. Here, we provide evidence that combining any member of the GLP1R agonist class with any member of the DYRK1A inhibitor class induces a synergistic increase in human β cell replication (5 to 6%) accompanied by an actual increase in numbers of human β cells. GLP1R agonist-DYRK1A inhibitor synergy required combined inhibition of DYRK1A and an increase in cAMP and did not lead to β cell dedifferentiation. These beneficial effects on proliferation were seen in both normal human β cells and β cells derived from individuals with type 2 diabetes. The ability of the GLP1R agonist-DYRK1A inhibitor combination to enhance human β cell proliferation, human insulin secretion, and blood glucose control extended in vivo to studies of human islets transplanted into euglycemic and streptozotocin-diabetic immunodeficient mice. No adverse events were observed in the mouse studies during a 1-week period. Because of the relative β cell specificity of GLP1R agonists, the combination provides an improved, although not complete, degree of human β cell specificity. |
Year of Publication |
2020
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Journal |
Science translational medicine
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Volume |
12
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Issue |
530
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Date Published |
02/2020
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ISSN Number |
1946-6242
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DOI |
10.1126/scitranslmed.aaw9996
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Alternate Journal |
Sci Transl Med
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PMID |
32051230
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PMCID |
PMC9945936
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