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miR-204 Controls Glucagon-Like Peptide 1 Receptor Expression and Agonist Function.

Citation
Jo, S. H., et al. “Mir-204 Controls Glucagon-Like Peptide 1 Receptor Expression And Agonist Function.”. Diabetes, pp. 256-264.
Center University of Alabama at Birmingham
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Author SeongHo Jo, Junqin Chen, Guanlan Xu, Truman B Grayson, Lance A Thielen, Anath Shalev
Abstract

Glucagon-like peptide 1 receptor (GLP1R) agonists are widely used to treat diabetes. However, their function is dependent on adequate GLP1R expression, which is downregulated in diabetes. GLP1R is highly expressed on pancreatic β-cells, and activation by endogenous incretin or GLP1R agonists increases cAMP generation, which stimulates glucose-induced β-cell insulin secretion and helps maintain glucose homeostasis. We now have discovered that the highly β-cell-enriched microRNA, miR-204, directly targets the 3' UTR of GLP1R and thereby downregulates its expression in the β-cell-derived rat INS-1 cell line and primary mouse and human islets. Furthermore, in vivo deletion of miR-204 promoted islet GLP1R expression and enhanced responsiveness to GLP1R agonists, resulting in improved glucose tolerance, cAMP production, and insulin secretion as well as protection against diabetes. Since we recently identified thioredoxin-interacting protein (TXNIP) as an upstream regulator of miR-204, we also assessed whether in vivo deletion of TXNIP could mimic that of miR-204. Indeed, it also enhanced islet GLP1R expression and GLP1R agonist-induced insulin secretion and glucose tolerance. Thus, the present studies show for the first time that GLP1R is under the control of a microRNA, miR-204, and uncover a previously unappreciated link between TXNIP and incretin action.

Year of Publication
2018
Journal
Diabetes
Volume
67
Issue
2
Number of Pages
256-264
Date Published
12/2018
ISSN Number
1939-327X
DOI
10.2337/db17-0506
Alternate Journal
Diabetes
PMID
29101219
PMCID
PMC5780066
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