Efficacy in diet‐induced obese mice of the hepatotropic, peripheral cannabinoid 1 receptor inverse agonist TM38837

利莫那班 减肥 大麻素受体 内科学 内分泌学 受体 医学 反激动剂 大麻素 兴奋剂 食欲 药理学 体温过低 肥胖
作者
Martin Cooper,Pia K. Nørregaard,Thomas Högberg,Gunnar Andersson,Jean‐Marie Receveur,Jean‐Michel Linget,Christian Elling
出处
期刊:British Journal of Pharmacology [Wiley]
卷期号:181 (20): 3926-3943
标识
DOI:10.1111/bph.16401
摘要

Background and Purpose The cannabinoid CB 1 receptor has a well‐established role in appetite regulation. Drugs antagonizing central CB 1 receptors, most notably rimonabant, induced weight loss and improved the metabolic profile in obese individuals but were discontinued due to psychiatric side effects. However, metabolic benefits were only partially attributable to weight loss, implying a role for peripheral receptors, and peripherally restricted CB 1 receptor antagonists have since been of interest. Herein, we describe the evaluation of the peripherally restricted potent CB 1 receptor inverse agonists TM38837 and TM39875, with acidic functionality, which were administered daily to diet‐induced obese (DIO) mice for 5 weeks at doses for which CNS‐mediated effects were minimal. Experimental Approach Compounds were tested in dose–response in acute studies to compare efficacy (gastric transport) and extent of CNS exposure (hypothermia and satiety sequence) to demonstrate peripheral restriction and select doses for the subsequent chronic DIO study. Key Results TM38837 but not TM39875 produced considerable (26%) weight loss, linked to a sustained reduction in food intake, together with improvements in plasma markers of inflammation and glucose homeostasis. Pharmacokinetic analysis indicated high plasma and low brain levels for both compounds with high liver levels for TM38837 (but not TM39875) due to hepatic uptake. Conclusion and Implications Weight loss and metabolic benefits of TM38837 are likely not CNS‐mediated but could be linked to enhanced liver exposure, which implicates intracellular CB 1 receptors in hepatocytes as a possible driver of obesity and co‐morbidities.
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