AM1638, a GPR40-Full Agonist, Inhibited Palmitate- Induced ROS Production and Endoplasmic Reticulum Stress, Enhancing HUVEC Viability in an NRF2-Dependent Manner

Hwan-jin Hwang; Joo Won Kim; Sukhwan Yun; Min Jeong Park; Eyun Song; Sooyeon Jang; Ahreum Jang; Kyung Mook Choi; Sei Hyun Baik; Hye Jin Yoo

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AM1638, a GPR40-Full Agonist, Inhibited Palmitate- Induced ROS Production and Endoplasmic Reticulum Stress, Enhancing HUVEC Viability in an NRF2-Dependent Manner

Author: Hwan-Jin HWANG ¹ ; Joo Won KIM ; SukHwan YUN ; Min Jeong PARK ; Eyun SONG ; Sooyeon JANG ; Ahreum JANG ; Kyung Mook CHOI ; Sei Hyun BAIK ; Hye Jin YOO
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1. BK21 Graduate Program, Department of Biomedical Sciences, Korea University College of Medicine, Seoul, Korea
Publication Type:Original Article
From:Endocrinology and Metabolism 2023;38(6):760-769
CountryRepublic of Korea
Language:English
Abstract: Background:G protein-coupled receptor 40 (GPR40) is a key molecule in diabetes and fatty liver, but its role in endothelial dysfunction remains unclear. Our objective in this study was to determine whether GPR40 agonists protect endothelial cells against palmitatemediated oxidative stress.
Methods:Human umbilical vein endothelial cells (HUVECs) were used to investigate effects of various GPR40 agonists on vascular endothelium.
Results:In HUVECs, AM1638, a GPR40-full agonist, enhanced nuclear factor erythroid 2–related factor 2 (NRF2) translocation to the nucleus and heme oxygenase-1 (HO-1) expression, which blocked palmitate-induced superoxide production. Those antioxidant effects were not detected after treatment with LY2922470 or TAK875, GPR40-partial agonists, suggesting that GPR40 regulates reactive oxygen species (ROS) removal in a ligand-dependent manner. We also found that palmitate-induced CCAAT/enhancer‐binding protein homologous protein expression; X-box binding protein-1 splicing, nuclear condensation, and fragmentation; and caspase-3 cleavage were all blocked in an NRF2-dependent manner after AM1638 treatment. Both LY2922470 and TAK875 also improved cell viability independent of the NRF2/ROS pathway by reducing palmitate-mediated endoplasmic reticulum stress and nuclear damage. GPR40 agonists thus have beneficial effects against palmitate in HUVECs. In particular, AM1638 reduced palmitate-induced superoxide production and cytotoxicity in an NRF2/HO-1 dependent manner.
Conclusion:GPR40 could be developed as a good therapeutic target to prevent or treat cardiovascular diseases such as atherosclerosis.