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Deletion of Gpr27 in vivo reduces insulin mRNA but does not result in diabetes.

Citation
Chopra, D. G., et al. “Deletion Of Gpr27 In Vivo Reduces Insulin Mrna But Does Not Result In Diabetes.”. Scientific Reports, p. 5629.
Author Deeksha G Chopra, Nicholas Yiv, Thomas G Hennings, Yaohuan Zhang, Gregory M Ku
Abstract

Gpr27 is a highly conserved, orphan G protein coupled receptor (GPCR) previously implicated in pancreatic beta cell insulin transcription and glucose-stimulated insulin secretion in vitro. Here, we characterize a whole-body mouse knockout of Gpr27. Gpr27 knockout mice were born at expected Mendelian ratios and exhibited no gross abnormalities. Insulin and Pdx1 mRNA in Gpr27 knockout islets were reduced by 30%, but this did not translate to a reduction in islet insulin content or beta cell mass. Gpr27 knockout mice exhibited slightly worsened glucose tolerance with lower plasma insulin levels while maintaining similar insulin tolerance. Unexpectedly, Gpr27 deletion reduced expression of Eif4e3, a neighboring gene, likely by deleting transcription start sites on the anti-sense strand of the Gpr27 coding exon. Our data confirm that loss of Gpr27 reduces insulin mRNA in vivo but has only minor effects on glucose tolerance.

Year of Publication
2020
Journal
Scientific reports
Volume
10
Issue
1
Number of Pages
5629
Date Published
03/2020
ISSN Number
2045-2322
DOI
10.1038/s41598-020-62358-4
Alternate Journal
Sci Rep
PMID
32221326
PMCID
PMC7101378
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