肝X受体
脂肪生成
餐后
血脂异常
内分泌学
以兹提米比
内科学
反激动剂
药理学
医学
胆固醇
兴奋剂
甘油三酯
脂质代谢
炎症
化学
胆固醇逆向转运
受体
微粒体甘油三酯转移蛋白
生物利用度
他汀类
糖尿病
PPAR激动剂
阿托伐他汀
低密度脂蛋白受体
核受体
脂肪肝
利拉鲁肽
作者
Xiaoxu Li,Giorgia Benegiamo,Archana Vijayakumar,NATALIE SRODA,Masaki Kimura,Ryan S. Huss,STEVE WENG,Eisuke Murakami,Brian J. Kirby,Giacomo V. G. von Alvensleben,Claus Kremoser,Edward Gane,Takanori Takebe,Robert P. Myers,G. Mani Subramanian,Johan Auwerx
出处
期刊:Nature Medicine
[Nature Portfolio]
日期:2026-01-16
卷期号:32 (3): 883-893
被引量:2
标识
DOI:10.1038/s41591-025-04169-6
摘要
Despite advances in lipid-lowering treatment, atherosclerotic cardiovascular disease remains the leading cause of mortality, underscoring the need to address residual risk. Targeting both the synthesis and clearance of triglyceride (TG)-rich lipoproteins is a promising approach. Liver X receptor (LXR) repression can reduce plasma TG and cholesterol and improve insulin sensitivity by suppressing de novo lipogenesis and intestinal lipid absorption and enhancing clearance of TG-rich lipoproteins, but its clinical utility remains unexplored. Here we demonstrate the role of LXR inverse agonists in lipid metabolism and metabolic diseases in preclinical models and humans. Given concerns that systemic LXR repression may impair reverse cholesterol transport, we developed TLC-2716, an orally administered, gut- and liver-restricted LXR inverse agonist. In human liver organoids modeling steatohepatitis, TLC-2716 reduced lipid accumulation and suppressed inflammation and fibrotic gene expression. In a randomized, placebo-controlled phase 1 clinical trial, 14-day treatment with TLC-2716 was well tolerated (primary endpoints) and resulted in placebo-adjusted reductions up to 38.5% in plasma TG and 61% in postprandial remnant cholesterol (secondary endpoints). In conclusion, these results highlight the tolerability and therapeutic potential of TLC-2716 as a treatment for managing dyslipidemia and reducing residual atherosclerotic cardiovascular disease risk in humans. ClinicalTrials.gov identifier: NCT05483998 .
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