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酰胺或胺:使用 15N 同位素标记确定蛋白质 SFG 光谱中 3300 cm(-1) NH 模式的来源。

Amide or amine: determining the origin of the 3300 cm(-1) NH mode in protein SFG spectra using 15N isotope labels.

出版信息

J Phys Chem B. 2009 Nov 26;113(47):15423-6. doi: 10.1021/jp908773c.

Abstract

Sum frequency generation (SFG) vibrational spectroscopy has been employed in biomaterials research and protein adsorption studies with growing success in recent years. A number of studies focusing on understanding SFG spectra of proteins and peptides at different interfaces have laid the foundation for future, more complex studies. In many cases, a strong NH mode near 3300 cm(-1) is observed in the SFG spectra, but the relationship of this mode to the peptide structure is uncertain, since it has been assigned to either a backbone amide mode or a side chain related amine resonance. A thorough understanding of the SFG spectra of these first model systems is an important first step for future experiments. To clarify the origin of the NH SFG mode, we studied (15)N isotopically labeled 14-amino acid amphiphilic model peptides composed of lysine (K) and leucine (L) in an alpha-helical secondary structure (LKalpha14) that were adsorbed onto charged surfaces in situ at the solid-liquid interface. (15)N substitution at the terminal amine group of the lysine side chains resulted in a red-shift of the NH mode of 9 cm(-1) on SiO(2) and 13 cm(-1) on CaF(2). This clearly shows the 3300 cm(-1) NH feature is associated with side chain NH stretches and not with backbone amide modes.

摘要

和频产生(SFG)振动光谱学近年来在生物材料研究和蛋白质吸附研究中取得了越来越大的成功。许多专注于理解不同界面处蛋白质和肽的 SFG 光谱的研究为未来更复杂的研究奠定了基础。在许多情况下,在 SFG 光谱中观察到在 3300cm-1 附近的强 NH 模式,但由于其被分配到肽链酰胺模式或侧链相关的胺共振,因此该模式与肽结构的关系不确定。彻底了解这些第一个模型系统的 SFG 光谱是未来实验的重要第一步。为了澄清 NH SFG 模式的起源,我们研究了在固-液界面原位吸附在带电表面上的具有α-螺旋二级结构的 14 个氨基酸两亲性模型肽(LKalpha14),该模型肽由赖氨酸(K)和亮氨酸(L)组成,并且(15)N 同位素标记了赖氨酸侧链的末端胺基。(15)N 在 SiO2 上取代赖氨酸侧链末端胺基导致 NH 模式红移 9cm-1,在 CaF2 上红移 13cm-1。这清楚地表明 3300cm-1 的 NH 特征与侧链 NH 伸展有关,而与肽链酰胺模式无关。

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