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Rat nicotinic ACh receptor α7 and β2 subunits co-assemble to form functional heteromeric nicotinic receptor channels

机译:大鼠烟碱型ACh受体α7和β2亚基共同组装形成功能性异烟碱样受体通道

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摘要

Rat hippocampal interneurons express diverse subtypes of functional nicotinic acetylcholine receptors (nAChRs), including α7-containing receptors that have properties unlike those expected for homomeric α7 nAChRs. We previously reported a strong correlation between expression of the α7 and of the β2 subunits in individual neurons. To explore whether co-assembly of the α7 and β2 subunits might occur, these subunits were co-expressed in Xenopus oocytes and the functional properties of heterologously expressed nAChRs were characterized by two-electrode voltage clamp. Co-expression of the β2 subunit, both wild-type and mutant forms, with the α7 subunit significantly slowed the rate of nAChR desensitization and altered the pharmacological properties. Whereas ACh, carbachol and choline were full or near-full agonists for homomeric α7 receptor channels, both carbachol and choline were only partial agonists in oocytes expressing both α7 and β2 subunits. In addition the EC50 values for all three agonists significantly increased when the β2 subunit was co-expressed with the α7 subunit. Co-expression with the β2 subunit did not result in any significant change in the current-voltage curve. Biochemical evidence for the co-assembly of the α7 and β2 subunits was obtained by co-immunoprecipitation of these subunits from transiently transfected human embryonic kidney (TSA201) cells. These data provide direct biophysical and molecular evidence that the nAChR α7 and β2 subunits co-assemble to form a functional heteromeric nAChR with functional and pharmacological properties different from those of homomeric α7 channels. This co-assembly may help to explain nAChR channel diversity in rat hippocampal interneurons, and perhaps in other areas of the nervous system.
机译:大鼠海马中间神经元表达功能性烟碱型乙酰胆碱受体(nAChRs)的各种亚型,包括具有与同源α7nAChRs不同的特性的含α7受体。我们先前曾报道单个神经元中α7和β2亚基的表达之间存在很强的相关性。为了探讨是否可能发生α7和β2亚基的共装配,这些亚基在非洲爪蟾卵母细胞中共表达,并通过两电极电压钳表征异源表达的nAChRs的功能特性。 β2亚基(野生型和突变型)与α7亚基的共表达显着减慢了nAChR脱敏的速率并改变了药理特性。尽管ACh,卡巴胆碱和胆碱是同源α7受体通道的完全或接近全效激动剂,但在表达α7和β2亚基的卵母细胞中,卡巴胆碱和胆碱仅是部分激动剂。此外,当β2亚基与α7亚基共表达时,所有三种激动剂的EC50值均显着增加。与β2亚基的共表达不会导致电流-电压曲线发生任何显着变化。通过从瞬时转染的人胚肾(TSA201)细胞中共免疫沉淀这些亚基,可以获得α7和β2亚基共装配的生化证据。这些数据提供了直接的生物物理和分子证据,表明nAChRα7和β2亚基共同组装形成功能性异源nAChR,其功能和药理特性不同于同型α7通道。这种共同组装可能有助于解释大鼠海马中间神经元以及神经系统其他区域的nAChR通道多样性。

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