| Literature DB >> 25918235 |
H Siebe Spijker1, Heein Song2, Johanne H Ellenbroek1, Maaike M Roefs1, Marten A Engelse1, Erik Bos3, Abraham J Koster3, Ton J Rabelink1, Barbara C Hansen4, Anne Clark5, Françoise Carlotti1, Eelco J P de Koning6.
Abstract
Loss of pancreatic islet β-cell mass and β-cell dysfunction are central in the development of type 2 diabetes (T2DM). We recently showed that mature human insulin-containing β-cells can convert into glucagon-containing α-cells ex vivo. This loss of β-cell identity was characterized by the presence of β-cell transcription factors (Nkx6.1, Pdx1) in glucagon(+) cells. Here, we investigated whether the loss of β-cell identity also occurs in vivo, and whether it is related to the presence of (pre)diabetes in humans and nonhuman primates. We observed an eight times increased frequency of insulin(+) cells coexpressing glucagon in donors with diabetes. Up to 5% of the cells that were Nkx6.1(+) but insulin(-) coexpressed glucagon, which represents a five times increased frequency compared with the control group. This increase in bihormonal and Nkx6.1(+)glucagon(+)insulin(-) cells was also found in islets of diabetic macaques. The higher proportion of bihormonal cells and Nkx6.1(+)glucagon(+)insulin(-) cells in macaques and humans with diabetes was correlated with the presence and extent of islet amyloidosis. These data indicate that the loss of β-cell identity occurs in T2DM and could contribute to the decrease of functional β-cell mass. Maintenance of β-cell identity is a potential novel strategy to preserve β-cell function in diabetes.Entities:
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Year: 2015 PMID: 25918235 DOI: 10.2337/db14-1752
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461