Department of Chemistry, University of California at Irvine, Irvine, California 92697-2025, USA.
J Phys Chem B. 2011 May 12;115(18):5168-82. doi: 10.1021/jp105527n. Epub 2010 Sep 16.
We have carried out structural determination of capped C(α,α)-diethylglycine (Deg) homopeptides with different chain lengths, Ac-(Deg)(n)-OtBu (n = 2-5), solvated in CDCl(3), and investigated vibrational properties of the amide I and II modes by linear and 2D IR spectroscopy, ONIOM calculations, and molecular dynamics simulations. 2D IR experiments were performed in the amide I region using the rephasing pulse sequence under the double-crossed polarization and the nonrephasing sequence under a new polarization configuration to measure cross-peak patterns in the off-diagonal regions. The 2D IR spectra measured in the amide I and II regions reveal complex couplings between these modes. Model spectral calculations finely reproduced the measured spectral profiles by using vibrational parameters that were very close to the values predicted by the ONIOM method. The agreement led to a conclusion that peptide backbones are fully extended with the dihedral angles (ϕ,ψ) ≈ (±180°,±180°) and that a sequence of intramolecular C(5) hydrogen bonds forms along the entire chain regardless of the chain length. This conclusion was endorsed by analysis of the molecular dynamics trajectories for n = 3 and 5 that showed an exclusive population of the C(5) conformation. The conformationally well-restrained Deg homopeptides serve as an ideal linear exciton chain, which is scarcely obtainable by protein amino acids. We investigated excitonic properties of the linear chain through analytic modeling and compared the measurement and calculation results of the amide I and II modes. The integrated intensity of the amide II band is larger than that of the amide I for the C(5) structure, untypical behavior in contrast with other secondary structures. This comprehensive study characterized the amide I and II spectral signatures of the fully extended conformation, which will facilitate the conformational analysis of artificial oligopeptides that contain such structural motifs.
我们已经对不同链长的封端 C(α,α)-二乙基甘氨酸 (Deg) 同聚肽,Ac-(Deg)(n)-OtBu(n = 2-5)进行了结构测定,这些同聚肽溶解在 CDCl(3) 中,并通过线性和 2D IR 光谱、ONIOM 计算和分子动力学模拟研究了酰胺 I 和 II 模式的振动特性。在酰胺 I 区域进行了 2D IR 实验,使用重相位脉冲序列在双交叉偏振下和新的偏振配置下的非重相位序列测量对角区域中的交叉峰图案。在酰胺 I 和 II 区域测量的 2D IR 光谱揭示了这些模式之间的复杂耦合。模型光谱计算通过使用非常接近 ONIOM 方法预测值的振动参数,精细地再现了测量的光谱轮廓。这种一致性得出的结论是,肽骨架完全伸展,二面角(ϕ,ψ)≈(±180°,±180°),并且无论链长如何,沿整个链形成一系列分子内 C(5)氢键。这一结论得到了 n = 3 和 5 的分子动力学轨迹分析的支持,该分析表明 C(5)构象的种群是独占的。构象约束良好的 Deg 同聚肽是一种理想的线性激子链,这在蛋白质氨基酸中很少见。我们通过分析建模研究了线性链的激子性质,并比较了酰胺 I 和 II 模式的测量和计算结果。对于 C(5)结构,酰胺 II 带的积分强度大于酰胺 I 的积分强度,这是与其他二级结构不同的非典型行为。这项综合研究表征了完全伸展构象的酰胺 I 和 II 光谱特征,这将有助于含有这种结构基序的人工寡肽的构象分析。
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