Sheffler Douglas J, Williams Richard, Bridges Thomas M, Xiang Zixiu, Kane Alexander S, Byun Nellie E, Jadhav Satyawan, Mock Mathew M, Zheng Fang, Lewis L Michelle, Jones Carrie K, Niswender Colleen M, Weaver Charles D, Lindsley Craig W, Conn P Jeffrey
Department of Pharmacology, Vanderbilt University Medical Center, Nashville, TN 37232, USA.
Mol Pharmacol. 2009 Aug;76(2):356-68. doi: 10.1124/mol.109.056531. Epub 2009 Apr 30.
Previous studies suggest that selective antagonists of specific subtypes of muscarinic acetylcholine receptors (mAChRs) may provide a novel approach for the treatment of certain central nervous system (CNS) disorders, including epileptic disorders, Parkinson's disease, and dystonia. Unfortunately, previously reported antagonists are not highly selective for specific mAChR subtypes, making it difficult to definitively establish the functional roles and therapeutic potential for individual subtypes of this receptor subfamily. The M(1) mAChR is of particular interest as a potential target for treatment of CNS disorders. We now report the discovery of a novel selective antagonist of M(1) mAChRs, termed VU0255035 [N-(3-oxo-3-(4-(pyridine-4-yl)piperazin-1-yl)propyl)-benzo[c][1,2,5]thiadiazole-4 sulfonamide]. Equilibrium radioligand binding and functional studies demonstrate a greater than 75-fold selectivity of VU0255035 for M(1) mAChRs relative to M(2)-M(5). Molecular pharmacology and mutagenesis studies indicate that VU0255035 is a competitive orthosteric antagonist of M(1) mAChRs, a surprising finding given the high level of M(1) mAChR selectivity relative to other orthosteric antagonists. Whole-cell patch-clamp recordings demonstrate that VU0255035 inhibits potentiation of N-methyl-D-aspartate receptor currents by the muscarinic agonist carbachol in hippocampal pyramidal cells. VU0255035 has excellent brain penetration in vivo and is efficacious in reducing pilocarpine-induced seizures in mice. We were surprised to find that doses of VU0255035 that reduce pilocarpine-induced seizures do not induce deficits in contextual freezing, a measure of hippocampus-dependent learning that is disrupted by nonselective mAChR antagonists. Taken together, these data suggest that selective antagonists of M(1) mAChRs do not induce the severe cognitive deficits seen with nonselective mAChR antagonists and could provide a novel approach for the treatment certain of CNS disorders.
先前的研究表明,毒蕈碱型乙酰胆碱受体(mAChRs)特定亚型的选择性拮抗剂可能为治疗某些中枢神经系统(CNS)疾病提供一种新方法,这些疾病包括癫痫疾病、帕金森病和肌张力障碍。不幸的是,先前报道的拮抗剂对特定mAChR亚型的选择性不高,这使得难以确切确定该受体亚家族各个亚型的功能作用和治疗潜力。M(1) mAChR作为CNS疾病治疗的潜在靶点尤其受到关注。我们现在报告发现了一种新型的M(1) mAChRs选择性拮抗剂,称为VU0255035 [N-(3-氧代-3-(4-(吡啶-4-基)哌嗪-1-基)丙基)-苯并[c][1,2,5]噻二唑-4-磺酰胺]。平衡放射性配体结合和功能研究表明,相对于M(2)-M(5),VU0255035对M(1) mAChRs的选择性大于75倍。分子药理学和诱变研究表明,VU0255035是M(1) mAChRs的竞争性正构拮抗剂,鉴于相对于其他正构拮抗剂而言,M(1) mAChR具有高度选择性,这一发现令人惊讶。全细胞膜片钳记录表明,VU0255035抑制毒蕈碱激动剂卡巴胆碱对海马锥体细胞中N-甲基-D-天冬氨酸受体电流的增强作用。VU0255035在体内具有出色的脑渗透性,并且在减少毛果芸香碱诱导的小鼠癫痫发作方面有效。我们惊讶地发现,降低毛果芸香碱诱导的癫痫发作的VU0255035剂量不会诱导情境性僵立缺陷,情境性僵立是一种衡量海马依赖性学习的指标,会被非选择性mAChR拮抗剂破坏。综上所述,这些数据表明,M(1) mAChRs的选择性拮抗剂不会诱导非选择性mAChR拮抗剂所导致的严重认知缺陷,并且可能为治疗某些CNS疾病提供一种新方法。
