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Secondary Ammonium Agonists Make Dual Cation-π Interactions in α4β2 Nicotinic Receptors

机译:仲铵激动剂在α4β2烟碱受体中产生双重阳离子-π相互作用

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摘要

A cation-π interaction between the ammonium group of an agonist and a conserved tryptophan termed TrpB is a near universal feature of agonist binding to nicotinic acetylcholine receptors (nAChRs). TrpB is one of five residues that form the aromatic box of the agonist binding site, and for the prototype agonists ACh and nicotine, only TrpB makes a functional cation-π interaction. We report that, in addition to TrpB, a significant cation-π interaction is made to a second aromatic, TyrC2, by the agonists metanicotine, TC299423, varenicline, and nornicotine. A common structural feature of these agonists, and a distinction from ACh and nicotine, is a protonated secondary amine that provides the cation for the cation-π interaction. These results indicate a distinction in binding modes between agonists with subtly different structures that may provide guidance for the development of subtype-selective agonists of nAChRs.
机译:激动剂的铵基和保守的色氨酸之间的阳离子-π相互作用称为TrpB,是激动剂与烟碱乙酰胆碱受体(nAChRs)结合的近乎普遍的特征。 TrpB是形成激动剂结合位点芳香盒的五个残基之一,而对于原型激动剂ACh和尼古丁,只有TrpB可以进行阳离子-π相互作用。我们报告说,除了TrpB之外,激动剂metanicotine,TC299423,varennicline和nornicotine还对第二种芳香族化合物TyrC2产生了显着的阳离子-π相互作用。这些激动剂的共同结构特征是质子化仲胺,它与ACh和尼古丁有区别,它为阳离子与π的相互作用提供阳离子。这些结果表明,在具有微妙不同结构的激动剂之间的结合方式上的区别,可以为nAChRs亚型选择性激动剂的开发提供指导。

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