A novel monoacylglycerol lipase-targeted 18F-labeled probe for positron emission tomography imaging of brown adipose tissue in the energy network

单酰甘油脂肪酶 内大麻素系统 丝氨酸水解酶 脂肪组织 2-花生四烯酸甘油 褐色脂肪组织 化学 生物化学 药理学 生物 丝氨酸 大麻素受体 受体 兴奋剂
作者
Ran Cheng,Masayuki Fujinaga,Jing Yang,Jian Rong,Ahmed Haider,Daisuke Ogasawara,Richard Van,Tuo Shao,Zhe Chen,Xiaofei Zhang,Erick R Calderon Leon,Yiding Zhang,Wakana Mori,Katsushi Kumata,Tomoteru Yamasaki,Lin Xie,Shi‐Gang Sun,Lu Wang,Chongzhao Ran,Yihan Shao,Benjamin F. Cravatt,Lee Josephson,Ming‐Rong Zhang,Steven H. Liang
出处
期刊:Acta pharmacologica Sinica [Springer Nature]
卷期号:43 (11): 3002-3010 被引量:2
标识
DOI:10.1038/s41401-022-00912-8
摘要

Monoacylglycerol lipase (MAGL) constitutes a serine hydrolase that orchestrates endocannabinoid homeostasis and exerts its function by catalyzing the degradation of 2-arachidonoylglycerol (2-AG) to arachidonic acid (AA). As such, selective inhibition of MAGL represents a potential therapeutic and diagnostic approach to various pathologies including neurodegenerative disorders, metabolic diseases and cancers. Based on a unique 4-piperidinyl azetidine diamide scaffold, we developed a reversible and peripheral-specific radiofluorinated MAGL PET ligand [18F]FEPAD. Pharmacokinetics and binding studies on [18F]FEPAD revealed its outstanding specificity and selectivity towards MAGL in brown adipose tissue (BAT) – a tissue that is known to be metabolically active. We employed [18F]FEPAD in PET studies to assess the abundancy of MAGL in BAT deposits of mice and found a remarkable degree of specific tracer binding in the BAT, which was confirmed by post-mortem tissue analysis. Given the negative regulation of endocannabinoids on the metabolic BAT activity, our study supports the concept that dysregulation of MAGL is likely linked to metabolic disorders. Further, we now provide a suitable imaging tool that allows non-invasive assessment of MAGL in BAT deposits, thereby paving the way for detailed mechanistic studies on the role of BAT in endocannabinoid system (ECS)-related pathologies.
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