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. 2025 Apr 24;68(8):8729-8767.
doi: 10.1021/acs.jmedchem.5c00402. Epub 2025 Apr 4.

Structure-Based Design and Optimization Lead to the Identification of a Novel Potent sEH Inhibitor with PPARγ Partial Agonist Activity against Inflammatory and Metabolic-Related Diseases

Ruolin Cao  1 Maoying Zhang  1 Minggang Qi  1 Zhen Zhang  1 Christophe Morisseau  2 Chunwei Zhou  3 Tianqi Sun  4 Junning Zhuang  1 Lu Chen  1 Cheng Xu  4 Zhongbo Liu  5 Bruce D Hammock  2 Guoliang Chen  1
Affiliations

Structure-Based Design and Optimization Lead to the Identification of a Novel Potent sEH Inhibitor with PPARγ Partial Agonist Activity against Inflammatory and Metabolic-Related Diseases

Ruolin Cao et al. J Med Chem. .

Abstract

The peroxisome proliferator-activated receptor-γ (PPARγ) serves as a pivotal regulator of lipid balance, adipogenesis, and inflammatory processes. PPARγ full agonists display strong curative effects but also serious adverse effects. Here, we found a novel 4-(cyclohexyloxy)phenyl acetate scaffold with partial PPARγ agonist activity, and its structure-activity relationship was studied. We also describe the structure-guided lead optimization of orally bioavailable SP-C01 as a dual modulator of soluble epoxide hydrolase (sEH) and partial PPARγ, which can inhibit Ser273 phosphorylation. In mice, oral administration of SP-C01 at a dose of 5 g/kg resulted in excellent safety; a significant reduction in the negative consequences of lipid accumulation and water-sodium retention; and no gastrointestinal adverse effects, weight gain, or cardiotoxicity. In addition, SP-C01 has shown a better effect than pioglitazone (Pio.) in type 2 diabetes and nonalcoholic steatohepatitis. Additionally, SP-C01 has demonstrated potent anti-inflammatory and analgesic properties in models of both neuropathic and inflammatory pain.

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Conflict of interest statement

Competing interests:

All other authors declare they have no competing interests conflict.

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