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跨膜区2(TM2)的疏水环在α9α10烟碱型胆碱能受体门控中的关键作用

Key roles of hydrophobic rings of TM2 in gating of the alpha9alpha10 nicotinic cholinergic receptor.

作者信息

Plazas Paola V, De Rosa María J, Gomez-Casati María E, Verbitsky Miguel, Weisstaub Noelia, Katz Eleonora, Bouzat Cecilia, Elgoyhen Ana Belén

机构信息

Instituto de Investigaciones en Ingeniería Genética y Biología Molecular, CONICET-UBA, Vuelta de Obligado 2490, Buenos Aires 1428, Argentina.

出版信息

Br J Pharmacol. 2005 Aug;145(7):963-74. doi: 10.1038/sj.bjp.0706224.

Abstract

We have performed a systematic mutagenesis of three hydrophobic rings (17', 13' and 9') within transmembrane region (TM) 2 of the alpha9alpha10 nicotinic cholinergic receptor (nAChR) to a hydrophilic (threonine) residue and compared the properties of mutant receptors reconstituted in Xenopus laevis oocytes. Phenotypic changes in alpha9alpha10 mutant receptors were evidenced by a decrease in the desensitization rate, an increase in both the EC(50) for ACh as well as the efficacy of partial agonists and the reduction of the allosteric modulation by extracellular Ca(2+). Mutated receptors exhibited spontaneous openings and, at the single-channel level, an increased apparent mean open time with no major changes in channel conductance, thus suggesting an increase in gating of the channel as the underlying mechanism. Overall, the degrees of the phenotypes of mutant receptors were more overt in the case of the centrally located V13'T mutant. Based on the atomic model of the pore of the electric organ of the Torpedo ray, we can propose that the interactions of side chains at positions 13' and 9' are key ones in creating an energetic barrier to ion permeation. In spite of the fact that the roles of the TM2 residues are mostly conserved in the distant alpha9alpha10 member of the nAChR family, their mechanistic contributions to channel gating show significant differences when compared to other nAChRs. These differences might be originated from slight differential intramolecular rearrangements during gating for the different receptors and might lead each nAChR to be in tune with their physiological roles.

摘要

我们对α9α10烟碱型胆碱能受体(nAChR)跨膜区(TM)2内的三个疏水环(17'、13'和9')进行了系统诱变,将其突变为亲水(苏氨酸)残基,并比较了在非洲爪蟾卵母细胞中重组的突变受体的特性。α9α10突变受体的表型变化表现为脱敏速率降低、乙酰胆碱(ACh)的半数有效浓度(EC50)以及部分激动剂的效能增加,以及细胞外Ca2+的变构调节作用减弱。突变受体表现出自发开放,在单通道水平上,表观平均开放时间增加,而通道电导没有重大变化,因此表明通道门控增加是其潜在机制。总体而言,在位于中心位置的V13'T突变体中,突变受体的表型程度更为明显。基于电鳐电器官孔的原子模型,我们可以提出,13'和9'位置的侧链相互作用是形成离子渗透能量屏障的关键因素。尽管TM2残基的作用在nAChR家族中距离较远的α9α10成员中大多是保守的,但与其他nAChR相比,它们对通道门控的机制贡献存在显著差异。这些差异可能源于不同受体门控过程中轻微的分子内重排差异,并可能导致每个nAChR与其生理作用相匹配。

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