1. Overexpression of intraislet ghrelin enhances β-cell proliferation after streptozotocin-induced β-cell injury in mice.
- Author
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Bando, Mika, Iwakura, Hiroshi, Ariyasu, Hiroyuki, Koyama, Hiroyuki, Hosoda, Kiminori, Adachi, Souichi, Nakao, Kazuwa, Kangawa, Kenji, and Akamizu, Takashi
- Subjects
STREPTOZOTOCIN ,GHRELIN receptors ,GLUCOSE metabolism ,CELL proliferation ,SOMATOTROPIN ,ACYLTRANSFERASES ,MESSENGER RNA - Abstract
Previously, we reported that exogenous administration of ghrelin ameliorates glucose metabolism in a neonate streptozotocin (STZ)- induced diabetic rat model through enhancement of β-cell proliferation. However, it was not clear whether the observed β-cell proliferation was a direct or indirect effect (e.g., via orexigenic or growth hormone-stimulated pathways) of ghrelin activity. Here, we aimed to investigate whether ghrelin directly impacts β-cell proliferation after STZ-induced injury in mice. Seven-week-old male rat insulin II promoter-ghrelin internal ribosomal sequence ghrelin O-acyltransferase transgenic (RIP-GG Tg) mice, which have elevated pancreatic ghrelin levels, but only minor changes in plasma ghrelin levels when fed a medium-chain triglyceride-rich diet, were treated with STZ. Then, serum insulin, pancreatic insulin mRNA expression, and islet histology were evaluated. We found that the serum insulin levels, but not blood glucose levels, of RIP-GG Tg mice were significantly ameliorated 14 days post-STZ treatment. Pancreatic insulin mRNA expression was significantly elevated in RIP-GG Tg mice, and β-cell numbers in islets were increased. Furthermore, the number of phos-phohistone H3
+ or Ki67+ proliferating β-cells was significantly elevated in RIP-GG Tg mice, whereas the apoptotic indexes within the islets, as determined by TUNEL assay, were not changed. These results indicate that ghrelin can directly stimulate β-cell proliferation in vivo after β-cell injury even without its orexigenic or GHstimulating activities, although it did not have enough impact to normalize the glucose tolerance in adult mice. [ABSTRACT FROM AUTHOR]- Published
- 2013
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