Frontiers in Pharmacology (Mar 2021)

The Effects of Apelin and Elabela Ligands on Apelin Receptor Distinct Signaling Profiles

  • Yunlu Jiang,
  • Maocai Yan,
  • Chunmei Wang,
  • Qinqin Wang,
  • Xiaoyu Chen,
  • Rumin Zhang,
  • Lei Wan,
  • Bingyuan Ji,
  • Bo Dong,
  • Huiyun Wang,
  • Jing Chen,
  • Jing Chen

DOI
https://doi.org/10.3389/fphar.2021.630548
Journal volume & issue
Vol. 12

Abstract

Read online

Apelin and Elabela are endogenous peptide ligands for Apelin receptor (APJ), a widely expressed G protein-coupled receptor. They constitute a spatiotemporal dual ligand system to control APJ signal transduction and function. We investigated the effects of Apelin-13, pGlu1-apelin-13, Apelin-17, Apelin-36, Elabela-21 and Elabela-32 peptides on APJ signal transduction. Whether different ligands are biased to different APJ mediated signal transduction pathways was studied. We observed the different changes of G protein dependent and β-arrestin dependent signaling pathways after APJ was activated by six peptide ligands. We demonstrated that stimulation with APJ ligands resulted in dose-dependent increases in both G protein dependent [cyclic AMP (cAMP), Ca2+ mobilization, and the early phase extracellular related kinase (ERK) activation] and β-arrestin dependent [GRKs, β-arrestin 1, β-arrestin 2, and β2 subunit of the clathrin adaptor AP2] signaling pathways. However, the ligands exhibited distinct signaling profiles. Elabela-32 showed a >1000-fold bias to the β-statin-dependent signaling pathway. These data provide that Apelin-17 was biased toward β-arrestin dependent signaling. Eabela-21 and pGlu1-Apelin-13 exhibited very distinct activities on the G protein dependent pathway. The activity profiles of these ligands could be valuable for the development of drugs with high selectivity for specific APJ downstream signaling pathways.

Keywords