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Identification of a small molecule activator of novel PKCs for promoting glucose-dependent insulin secretion
被引:0
|作者:
Shuai Han
Heling Pan
Jianhua Zhang
Li Tan
Dawei Ma
Junying Yuan
Jia-Rui Wu
机构:
[1] Key Laboratory of Systems Biology,Department of Cell Biology
[2] Institute of Biochemistry and Cell Biology,undefined
[3] Shanghai Institutes for Biological Sciences,undefined
[4] Chinese Academy of Sciences,undefined
[5] Shanghai Institute of Organic Chemistry,undefined
[6] Chinese Academy of Sciences,undefined
[7] Harvard Medical School,undefined
[8] Hefei National Laboratory for Physical Sciences at Microscale and School of Life Sciences,undefined
[9] University of Science & Technology of China,undefined
来源:
关键词:
PKC;
insulin secretion;
glucose dependency;
Golgi;
D O I:
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学科分类号:
摘要:
Using an image-based screen for small molecules that can affect Golgi morphology, we identify a small molecule, Sioc145, which can enlarge the Golgi compartments and promote protein secretion. More importantly, Sioc145 potentiates insulin secretion in a glucose-dependent manner. We show that Sioc145 selectively activates novel protein kinase Cs (nPKCs; δ and ɛ) but not conventional PKCs (cPKCs; α, βI and βII) in INS-1E insulinoma cells. In contrast, PMA, a non-selective activator of cPKCs and nPKCs, promotes insulin secretion independent of glucose concentrations. Furthermore, we demonstrate that Sioc145 and PMA show differential abilities in depolarizing the cell membrane, and suggest that Sioc145 promotes insulin secretion in the amplifying pathway downstream of KATP channels. In pancreatic islets, the treatment with Sioc145 enhances the second phase of insulin secretion. Increased insulin granules close to the plasma membrane are observed after Sioc145 treatment. Finally, the administration of Sioc145 to diabetic GK rats increases their serum insulin levels and improves glucose tolerance. Collectively, our studies identify Sioc145 as a novel glucose-dependent insulinotropic compound via selectively activating nPKCs.
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页码:588 / 599
页数:11
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