Gotti C, Carbonnelle E, Moretti M, Zwart R, Clementi F
Department of Medical Pharmacology, CNR Cellular and Molecular Pharmacology Center, University of Milan, Italy.
Behav Brain Res. 2000 Aug;113(1-2):183-92. doi: 10.1016/s0166-4328(00)00212-6.
Nicotine exerts a number of different effects on the nervous system by interacting with neuronal nicotinic acetylcholine receptors (nAChRs). These effects are mediated by its interaction with different nAChR subtypes, and this has led to the finding of subtype specific agonists and antagonists. In the search for subtype-selective drugs, we have synthesized some compounds derived from 4-oxystilbene, two of which (MG624 and F3) are selective ligands for the chick neuronal alphaBgtx receptors containing the alpha7 and/or alpha8 subunits. They have an antagonist action on oocyte-expressed chick and rat alpha7 subtypes. These compounds are selective toward the alpha7-containing receptors in chick, but, in mammals, although they still retain their potency toward alpha7-containing receptors, they are also active in non-alpha7-containing receptors.
尼古丁通过与神经元烟碱型乙酰胆碱受体(nAChRs)相互作用,对神经系统产生多种不同影响。这些影响是由其与不同nAChR亚型的相互作用介导的,这导致了亚型特异性激动剂和拮抗剂的发现。在寻找亚型选择性药物的过程中,我们合成了一些源自4-氧代二苯乙烯的化合物,其中两种(MG624和F3)是含有α7和/或α8亚基的鸡神经元αBgtx受体的选择性配体。它们对卵母细胞表达的鸡和大鼠α7亚型具有拮抗作用。这些化合物对鸡体内含α7的受体具有选择性,但在哺乳动物中,尽管它们对含α7的受体仍保持效力,但它们在不含α7的受体中也有活性。
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