Small molecule kaempferol modulates PDX-1 protein expression and subsequently promotes pancreatic ß-cell survival and function via CREB
Zhang YL, etc
Journal of Nutritional Biochesmitry,
2012
Chronic hyperlipidemia causes ß-cell apoptosis and dysfunction, thereby contributing to the pathogenesis of T2D. Thus, searching for agents to promote pancreatic ß-cell survival and improve its function could be a promising strategy to prevent and treat T2D. We investigated the effects of kaempferol, a small molecule isolated from ginkgo biloba, on apoptosis and function of ß-cells and further determined the mechanism underlying its actions. Kaempferol treatment promoted viability, inhibited apoptosis, and reduced caspase-3 activity in INS-1E cells and human islets chronically exposed to palmitate. In addition, kaempferol prevented the lipotoxicity-induced down-regulation of anti-apoptotic proteins Akt and Bcl-2. The cytoprotective effects of kaempferol were associated with improved insulin secretion, synthesis, and PDX-1 expression. Chronic hyperlipidemia significantly diminished cAMP production, PKA activation, and CREB phosphorylation and its regulated transcriptional activity in ß-cells, all of which were restored by kaempferol treatment. Disruption of CREB expression by transfection of CREB siRNA in INS-1E cells or adenoviral transfer of dominant-negative forms of CREB in human islets ablated kaempferol protection of ß-cell apoptosis and dysfunction caused by palmitate. Incubation of INS-1E cells or human islets with kaempferol for 48 h induced PDX-1 expression. This effect of kaempferol on PDX-1 expression was not shared by a host of structurally related flavonoid compounds. PDX-1 gene knockdown reduced kaempferol–stimulated cAMP generation and CREB activation in INS-1E cells. These findings demonstrate that kaempferol is a novel survivor factor for pancreatic ß-cells via up-regulating the PDX-1/cAMP/PKA/CREB signaling cascade.
- Journal
- Journal of Nutritional Biochesmitry
- Year
- 2012
- Page
- doi:10.1016/j.jnutbio.2012.03.008
- Institute
- Virginia Tech
Referenced Products
Product | Cat No. |
---|---|
Ad-pRL-Luc | 1671 |
Ad-CRE-Luc | 1672 |
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