Nature Communications (Dec 2024)

OSGEP regulates islet β-cell function by modulating proinsulin translation and maintaining ER stress homeostasis in mice

  • Yujie Liu,
  • Xuechun Yang,
  • Jian Zhou,
  • Haijun Yang,
  • Ruimeng Yang,
  • Peng Zhu,
  • Rong Zhou,
  • Tianyuan Wu,
  • Yongchao Gao,
  • Zhi Ye,
  • Xi Li,
  • Rong Liu,
  • Wei Zhang,
  • Honghao Zhou,
  • Qing Li

DOI
https://doi.org/10.1038/s41467-024-54905-8
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 19

Abstract

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Abstract Proinsulin translation and folding is crucial for glucose homeostasis. However, islet β-cell control of Proinsulin translation remains incompletely understood. Here, we identify OSGEP, an enzyme responsible for t6A37 modification of tRNANNU that tunes glucose metabolism in β-cells. Global Osgep deletion causes glucose intolerance, while β-cell-specific deletion induces hyperglycemia and glucose intolerance due to impaired insulin activity. Transcriptomics and proteomics reveal activation of the unfolded protein response (UPR) and apoptosis signaling pathways in Osgep-deficient islets, linked to an increase in misfolded Proinsulin from reduced t6A37 modification. Osgep overexpression in pancreas rescues insulin secretion and mitigates diabetes in high-fat diet mice. Osgep enhances translational fidelity and alleviates UPR signaling, highlighting its potential as a therapeutic target for diabetes. Individuals carrying the C allele at rs74512655, which promotes OSGEP transcription, may show reduced susceptibility to T2DM. These findings show OSGEP is essential for islet β-cells and a potential diabetes therapy target.