Molles Brian E, Tsigelny Igor, Nguyen Phuong D, Gao Sarah X, Sine Steven M, Taylor Palmer
Department of Pharmacology, Biomedical Sciences Graduate Program, University of California at San Diego, La Jolla, CA92093-0636, USA.
Biochemistry. 2002 Jun 25;41(25):7895-906. doi: 10.1021/bi025732d.
Waglerin-1 (Wtx-1) is a 22-amino acid peptide that competitively antagonizes muscle nicotinic acetylcholine receptors (nAChRs). Previous work demonstrated that Wtx-1 binds to mouse nAChRs with higher affinity than receptors from rats or humans, and distinguished residues in alpha and epsilon subunits that govern the species selectivity. These studies also showed that Wtx-1 binds selectively to the alpha-epsilon binding site with significantly higher affinity than to the alpha-delta binding site. Here we identify residues at equivalent positions in the epsilon, gamma, and delta subunits that govern Wtx-1 selectivity for one of the two binding sites on the nAChR pentamer. Using a series of chimeric and point mutant subunits, we show that residues Gly-57, Asp-59, Tyr-111, Tyr-115, and Asp-173 of the epsilon subunit account predominantly for the 3700-fold higher affinity of the alpha-epsilon site relative to that of the alpha-gamma site. Similarly, we find that residues Lys-34, Gly-57, Asp-59, and Asp-173 account predominantly for the high affinity of the alpha-epsilon site relative to that of the alpha-delta site. Analysis of combinations of point mutations reveals that Asp-173 in the epsilon subunit is required together with the remaining determinants in the epsilon subunit to achieve Wtx-1 selectivity. In particular, Lys-34 interacts with Asp-173 to confer high affinity, resulting in a DeltaDeltaG(INT) of -2.3 kcal/mol in the epsilon subunit and a DeltaDeltaG(INT) of -1.3 kcal/mol in the delta subunit. Asp-173 is part of a nonhomologous insertion not found in the acetylcholine binding protein structure. The key role of this insertion in Wtx-1 selectivity indicates that it is proximal to the ligand binding site. We use the binding and interaction energies for Wtx-1 to generate structural models of the alpha-epsilon, alpha-gamma, and alpha-delta binding sites containing the nonhomologous insertion.
瓦格勒毒素-1(Wtx-1)是一种由22个氨基酸组成的肽,它能竞争性拮抗肌肉型烟碱型乙酰胆碱受体(nAChRs)。先前的研究表明,Wtx-1与小鼠nAChRs的结合亲和力高于大鼠或人类的受体,并区分了决定物种选择性的α和ε亚基中的残基。这些研究还表明,Wtx-1选择性地结合到α-ε结合位点,其亲和力显著高于α-δ结合位点。在此,我们确定了ε、γ和δ亚基中对应位置的残基,这些残基决定了Wtx-1对nAChR五聚体上两个结合位点之一的选择性。通过一系列嵌合和点突变亚基,我们发现ε亚基的甘氨酸-57、天冬氨酸-59、酪氨酸-111、酪氨酸-115和天冬氨酸-173残基主要导致α-ε位点相对于α-γ位点的亲和力高3700倍。同样,我们发现赖氨酸-34、甘氨酸-57、天冬氨酸-59和天冬氨酸-173残基主要导致α-ε位点相对于α-δ位点的高亲和力。对组合点突变的分析表明,ε亚基中的天冬氨酸-173与ε亚基中的其余决定因素共同作用,以实现Wtx-1的选择性。特别是,赖氨酸-34与天冬氨酸-173相互作用以赋予高亲和力,导致ε亚基中的ΔΔG(INT)为-2.3千卡/摩尔,δ亚基中的ΔΔG(INT)为-1.3千卡/摩尔。天冬氨酸-173是乙酰胆碱结合蛋白结构中未发现的非同源插入序列的一部分。该插入序列在Wtx-1选择性中的关键作用表明它靠近配体结合位点。我们利用Wtx-1的结合和相互作用能生成包含非同源插入序列的α-ε、α-γ和α-δ结合位点的结构模型。
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