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Article Abstract

With the improvement of living standards, metabolic-disorder-associated steatohepatitis (MASH) has posed a serious threat to public health. In 2024, THR-β agonist was approved by the FDA as the first market drug for the treatment of MASH. In this work, we discovered a new class of THR-β agonists through structure-based rational design. Compound exhibited much higher agonistic activity (EC = 11.0 nM) and higher selectivity for THR-β over THR-α (THR-β/α = 34.1) compared to the market drug . More importantly, good pharmacokinetic properties of was observed with an excellent liver to heart ratio of 335:1. Notably, compound exhibited superior ability to improve steatosis, ballooning, inflammation and fibrosis, while did not show any improvement in inflammation, suggesting that is a highly promising THR-β agonist and warrants extensive preclinical investigation as a potential clinical development candidate for the treatment of MASH.

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http://dx.doi.org/10.1021/acs.jmedchem.5c00994DOI Listing

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