Peripherally restricted CB1 receptor blockers

被引:76
作者
Chorvat, Robert J. [1 ]
机构
[1] Jenrin Discovery, Wilmington, DE 19810 USA
关键词
Cannabinoid receptor blocker; Inverse agonist; Silent antagonist; Peripherally restricted CB1-antagonist; Obesity; Diabetes; Metabolic disorders; Liver diseases; Rimonabant; AM6545; JD5037; CARDIOMETABOLIC RISK-FACTORS; P-GLYCOPROTEIN EFFLUX; CANNABINOID RECEPTOR; INVERSE AGONIST; BODY-WEIGHT; BRAIN PENETRATION; ENDOCANNABINOID SYSTEM; INSULIN-RESISTANCE; RATIONAL DESIGN; ANTAGONISTS;
D O I
10.1016/j.bmcl.2013.06.066
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Antagonists (inverse agonists) of the cannabinoid-1 (CB1) receptor showed promise as new therapies for controlling obesity and related metabolic function/liver disease. These agents, representing diverse chemical series, shared the property of brain penetration due to the initial belief that therapeutic benefit was mainly based on brain receptor interaction. However, undesirable CNS-based side effects of the only marketed agent in this class, rimonabant, led to its removal, and termination of the development of other clinical candidates soon followed. Re-evaluation of this approach has focused on neutral or peripherally restricted (PR) antagonists. Supporting these strategies, pharmacological evidence indicates most if not all of the properties of globally acting agents may be captured by molecules with little brain presence. Methodology that can be used to eliminate BBB penetration and the means (in vitro assays, tissue distribution and receptor occupancy determinations, behavioral paradigms) to identify potential agents with little brain presence is discussed. Focus will be on the pharmacology supporting the contention that reported agents are truly peripherally restricted. Notable examples of these types of compounds are: TM38837 (structure not disclosed); AM6545 (8); JD5037 (15b); RTI-12 (19). (C) 2013 Elsevier Ltd. All rights reserved.
引用
收藏
页码:4751 / 4760
页数:10
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