ABT-089: Pharmacological Properties of a Neuronal Nicotinic Acetylcholine Receptor Agonist for the Potential Treatment of Cognitive Disorders

Lynne E. Rueter, David J. Anderson, Clark A. Briggs, Diana L. Donnelly-Roberts, Gary A. Gintant, Murali Gopalakrishnan, Nan-Horng Lin, Mark A. Osinski, Glenn A. Reinhart, Michael J. Buckley, Ruth L. Martin, Jeffrey S. McDermott, Lee C. Preusser, Terese R. Seifert, Zhi Su, Bryan F. Cox, Michael W. Decker, James P. Sullivan
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引用次数: 63

Abstract

ABT-089 [2-methyl-3-(2-(S)-pyrrolidinylmethoxy)pyridine dihydrochloride salt] is a selective neuronal nicotinic receptor (NNR) modulator with cognitive enhancing properties in animal models of cognitive functioning. Amongst NNR subtypes, ABT-089 shows selectivity for the cytisine binding site on the α4β2 receptor subtype as compared to the α-bungarotoxin (α-BgT) binding sites on the α7 and α1β1δγ receptor subtypes. In functional in vitro electrophysiological and cation flux assays, ABT-089 displays differential activity including agonism, partial agonism and antagonism depending upon the NNR subtype and assay. ABT-089 is as potent and efficacious as (–)-nicotine at evoking acetylcholine (ACh) release from hippocampal synaptosomes. Furthermore, ABT-089 is neuroprotective against excitotoxic glutamate insults, with even greater potency seen after chronic treatment. Similarly, ABT-089 is effective in models of cognitive functioning, including enhancement of baseline functioning as well as improvement of impaired cognitive functioning seen following septal lesioning and natural aging. In neuroprotective assays the compound is most potent by chronic administration. In stark contrast to the positive effects in the cognitive models, ABT-089 shows little propensity to induce adverse

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ABT-089:神经烟碱乙酰胆碱受体激动剂治疗认知障碍的药理特性
ABT-089[2-甲基-3-(2-(S)-吡咯烷基甲氧基)吡啶二盐酸盐]是一种选择性神经元烟碱受体(NNR)调节剂,在认知功能动物模型中具有认知增强特性。在NNR亚型中,ABT-089对α4β2受体亚型上的胱氨酸结合位点具有选择性,而对α7和α1β1δγ受体亚型上的α-bungarotoxin (α-BgT)结合位点具有选择性。在功能性体外电生理和阳离子通量试验中,ABT-089显示出不同的活性,包括激动作用、部分激动作用和拮抗作用,这取决于NNR亚型和试验。ABT-089在诱导海马突触体释放乙酰胆碱(ACh)方面与(-)-尼古丁一样有效。此外,ABT-089对兴奋毒性谷氨酸损伤具有神经保护作用,慢性治疗后的效力更大。同样,ABT-089在认知功能模型中是有效的,包括增强基线功能以及改善室间隔损伤和自然衰老后受损的认知功能。在神经保护试验中,慢性给药是最有效的。与认知模型中的积极作用形成鲜明对比的是,ABT-089几乎没有诱发不良反应的倾向
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