Ginsenoside F2 Restrains Hepatic Steatosis and Inflammation by Altering the Binding Affinity of Liver X Receptor Coregulators

Kyurae Kim; Myung-Ho Kim; Ji In Kang; Jong-In Baek; Byeong-Min Jeon; Ho Min Kim; Sun-Chang Kim; Won-Il Jeong

doi:10.1016/j.jgr.2023.10.001

Ginsenoside F2 Restrains Hepatic Steatosis and Inflammation by Altering the Binding Affinity of Liver X Receptor Coregulators

J Ginseng Res. 2024 Jan;48(1):89-97. doi: 10.1016/j.jgr.2023.10.001. Epub 2023 Oct 27.

Authors

Kyurae Kim¹, Myung-Ho Kim^{1

2}, Ji In Kang^{3

4}, Jong-In Baek^{5

6}, Byeong-Min Jeon^{5

6}, Ho Min Kim^{3

7}, Sun-Chang Kim^{5

6

8}, Won-Il Jeong^{1

9}

Affiliations

¹ Laboratory of Liver Research, Graduate School of Medical Science and Engineering, KAIST, Daejeon, Republic of Korea.
² Department of Internal Korean Medicine, Woosuk University Medical Center, Jeonju, Republic of Korea.
³ Biomedical Science and Engineering Interdisciplinary Program, KAIST, Daejeon, Republic of Korea.
⁴ Division of Oncology, Department of Medicine, Stanford University School of Medicine, Stanford, California, USA.
⁵ Department of Biological Sciences, KAIST, Daejeon, Republic of Korea.
⁶ Intelligent Synthetic Biology Center, Daejeon, Republic of Korea.
⁷ Center for Biomolecular and Cellular Structure, Institute for Basic Science (IBS), Daejeon, Republic of Korea.
⁸ KAIST Institutes, KAIST, Daejeon, Republic of Korea.
⁹ Center for the Hepatic Glutamate and Its Function, KAIST, Daejeon, Republic of Korea.

Abstract

Background: Ginsenoside F2 (GF2), the protopanaxadiol-type constituent in Panax ginseng, has been reported to attenuate metabolic dysfunction-associated steatotic liver disease (MASLD). However, the mechanism of action is not fully understood. Here, this study investigates the molecular mechanism by which GF2 regulates MASLD progression through liver X receptor (LXR).

Methods: To demonstrate the effect of GF2 on LXR activity, computational modeling of protein-ligand binding, Time-resolved fluorescence resonance energy transfer (TR-FRET) assay for LXR cofactor recruitment, and luciferase reporter assay were performed. LXR agonist T0901317 was used for LXR activation in hepatocytes and macrophages. MASLD was induced by high-fat diet (HFD) feeding with or without GF2 administration in WT and LXRα^-/- mice.

Results: Computational modeling showed that GF2 had a high affinity with LXRα. LXRE-luciferase reporter assay with amino acid substitution at the predicted ligand binding site revealed that the S264 residue of LXRα was the crucial interaction site of GF2. TR-FRET assay demonstrated that GF2 suppressed LXRα activity by favoring the binding of corepressors to LXRα while inhibiting the accessibility of coactivators. In vitro, GF2 treatments reduced T0901317-induced fat accumulation and pro-inflammatory cytokine expression in hepatocytes and macrophages, respectively. Consistently, GF2 administration ameliorated hepatic steatohepatitis and improved glucose or insulin tolerance in WT but not in LXRα^-/- mice.

Conclusion: GF2 alters the binding affinities of LXRα coregulators, thereby interrupting hepatic steatosis and inflammation in macrophages. Therefore, we propose that GF2 might be a potential therapeutic agent for the intervention in patients with MASLD.

Keywords: ginsenoside F2; liver X receptors; metabolic dysfunction-associated steatotic liver disease; nuclear receptor coactivator; nuclear receptor corepressor.