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Ligand-Induced Conformational Heterogeneity of Cytochrome P450 CYP119 Identified by 2D NMR Spectroscopy with the Unnatural Amino Acid 13C-p-Methoxyphenylalanine

机译:细胞色素P450 CYP119的配体诱导的构象异质性通过非天然氨基酸13C-p-甲氧基苯基丙氨酸的二维NMR光谱鉴定

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摘要

Conformational dynamics are thought to play an important role in ligand binding and catalysis by cytochrome P450 enzymes but few techniques exist to examine them in molecular detail. Using a unique isotopic labeling strategy, we have site specifically inserted a 13C-labeled unnatural amino acid residue, 13C-p-methoxyphenylalanine (MeOF), into two different locations in the substrate binding region of the thermophilic cytochrome P450 enzyme CYP119. Surprisingly, in both cases the resonance signal from the ligand-free protein is represented by a doublet in the 1H,13C-HSQC spectrum. Upon binding of 4-phenylimidazole, the signals from the initial resonances are reduced in favor a single new resonance, in the case of the F162MeOF mutant, or two new resonances, in the case of the F153MeOF mutant. This represents the first direct physical evidence for the ligand-dependent existence of multiple P450 conformers simultaneously in solution. This general approach may be used to further illuminate the role that conformational dynamics plays in the complex enzymatic phenomena exhibited by P450 enzymes.
机译:构象动力学被认为在细胞色素P450酶的配体结合和催化中起着重要作用,但是很少有技术可以对它们进行分子细节研究。使用独特的同位素标记策略,我们将一个 13 C标记的非天然氨基酸残基 13 Cp-甲氧基苯丙氨酸(MeOF)专门插入了该区域的两个不同位置嗜热细胞色素P450酶CYP119的底物结合区。出乎意料的是,在两种情况下,来自无配体蛋白的共振信号均由 1 H, 13 C-HSQC谱中的双峰表示。在结合4-苯基咪唑时,对于F162MeOF突变体,来自初始共振的信号减少,有利于单个新共振,对于F153MeOF突变体,有利于两个新共振。这代表了溶液中同时存在多个P450构象异构体的配体依赖性的第一个直接物理证据。这种通用方法可用于进一步阐明构象动力学在P450酶表现出的复杂酶促现象中的作用。

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