Avian fatty liver disease is a metabolic disease characterized by hepatocellular steatosis caused by fat deposition due to lipid metabolism disorders in poultry. AdipoRon, an adiponectin receptor agonist, has various biological effects, such as regulating glucose and lipid metabolism disorders, increasing insulin sensitivity, improving liver fat accumulation, and preventing inflammation and oxidative stress. Our previous study revealed that AdipoRon protected against liver injury induced by a high-fat diet and lipopolysaccharide in poultry. In this study, leghorn male hepatoma (LMH) cells were used to construct a lipotoxic injury model with mixed fatty acids (oleic acid + palmitic acid), and AdipoRon was subsequently used to intervene, followed by inhibition and activation of AMPK signaling pathways using an antagonist and agonist of AMPK, respectively, to detect lipid content and lipid deposition, hepatocyte injury-related transaminase activity, and the expression levels of lipid metabolism-related genes and key signaling molecules that regulate lipid metabolism, as well as the cellular lipid composition in LMH cells. AdipoRon promoted fatty acid oxidation, reduced lipid synthesis and deposition, and alleviated mixed fatty acid-induced lipotoxic injury through the regulation of the expression of adiponectin receptors, AMPK, PPARα, and key genes involved in lipid metabolism. The inhibition or activation of AMPK signaling pathways could regulate the expression of AdipoR1, AdipoR2, AMPK and p-AMPK, thereby altering the expression of lipid metabolism-related genes and antagonizing or synergistically increasing the ameliorative effects of AdipoRon on cellular lipid metabolism disorders, lipid deposition and cell injury. Lipidomic analysis further suggested that AdipoRon could regulate the metabolism of lipids such as sphingolipids, glycerophospholipids, acylcarnitines, and glycerolipids; reduce the accumulation of lipids such as ceramides, sphingomyelins, triacylglycerol, and acylcarnitines; maintain the metabolic homeostasis of phosphatidylamine and phosphatidylcholine, as well as cell membrane structural integrity and functional stability; and mitigate lipotoxic injury in LMH cells. This study provides new insights into targeted interventions involving adiponectin and its receptors to prevent and treat avian fatty liver disease.

01 Mar 2026·POULTRY SCIENCE

Protection of goose adiponectin-derived peptide gADP3 on LPS-induced thymus and spleen injury in goose

Article

Author: Ma, Ben ; Zheng, Yan ; Luan, Xinhong ; Yao, Zelong ; Cao, Zhongzan ; Gao, Ming

This study aims to evaluate the protective effects of goose-derived adiponectin peptide gADP3 on Lipopolysaccharide (LPS)-induced damage to goose thymus and spleen. LPS-induced inflammation was induced via intraperitoneal injection, with interventions using gADP3 and AdipoRon (positive control). Pathological changes in thymus and spleen tissues were observed. Levels of biochemical indicators related to inflammation, oxidative stress, and immunity in blood and tissue were measured. Additionally, tissue expression of key factors associated with inflammation, adiponectin receptors, and signaling pathways involved in inflammation and oxidative stress was assessed. The results showed that gADP3 and AdipoRon improved the histology of the thymus and spleen, reduced the infiltration of inflammatory cells, decreased the levels of the proinflammatory factors IL-6 and TNF-α, increased the levels of the anti-inflammatory factor IL-10, and alleviated the immune inflammatory responses induced by LPS. They also reduced the content of MDA in thymus and spleen tissues and enhanced GSH-Px activity in the thymus, thereby improving the status of oxidative stress. In terms of molecular mechanisms, both gADP3 and AdipoRon restored AdipoR1 mRNA expression and increased AMPK mRNA levels in the thymus. AdipoRon also restored AMPK protein levels. In the spleen, AdipoRon increased the expression of both AdipoR1 mRNA and protein, while gADP3 increased the mRNA expression of both AdipoR2 and AMPK. Furthermore, this study also found that LPS stimulation significantly upregulated the mRNA expression levels of NF-κB p65, MyD88, and TLR4 in the thymus, and markedly increased MyD88 protein levels. gADP3 and AdipoRon interventions significantly reduced mRNA and protein expression levels of these molecules. In spleen tissue, LPS stimulation significantly upregulated TLR4 mRNA levels and markedly increased NF-κB p65 and MyD88 protein levels, while gADP3 and AdipoRon interventions significantly reduced mRNA and protein expression levels of these molecules. In summary, our findings reveal that gADP3 alleviates immune and inflammatory damage in thymus and spleen tissues, thereby maintaining immune homeostasis in goslings and producing effects similar to those of AdipoRon.

01 Jan 2026·EUROPEAN JOURNAL OF PHARMACOLOGY

Corrigendum to “AdipoRon ameliorates anxiety- and depression-like behaviors in chronic restraint-stressed mice via AMPK-PPARα-BDNF-TrkB signaling” [Eur. J. Pharmacol. (2026) 1011 178468 doi: 10.1016/j.ejphar.2025.178468]

Author: Han, S ; Zeng, W ; Xie, T ; Wang, H ; Ma, L ; Zhang, Z ; Li, Y ; Hu, C ; Song, K ; Hashimoto, K ; Xie, H

100 Deals associated with AdipoRon

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Indication	Highest Phase	Country/Location	Organization	Date
Breast Cancer	Preclinical	China	National Taiwan University College of Medicine	28 Apr 2025
Diabetic Cardiomyopathies	Preclinical	South Korea	The Catholic University of Korea	06 Jun 2020
Type 2 diabetes mellitus with established diabetic nephropathy	Preclinical	South Korea	The Catholic University of Korea	31 Oct 2017
Diabetes Mellitus, Type 2	Preclinical	Japan	University of Tokyo	30 Oct 2013
Obesity	Preclinical	Japan	University of Tokyo	30 Oct 2013

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