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二维和频产生揭示了表面结合肽的结构与动力学。

Two-dimensional sum-frequency generation reveals structure and dynamics of a surface-bound peptide.

作者信息

Laaser Jennifer E, Skoff David R, Ho Jia-Jung, Joo Yongho, Serrano Arnaldo L, Steinkruger Jay D, Gopalan Padma, Gellman Samuel H, Zanni Martin T

机构信息

Department of Chemistry and ‡Department of Materials Science and Engineering, University of Wisconsin-Madison , Madison, Wisconsin 53706, United States.

出版信息

J Am Chem Soc. 2014 Jan 22;136(3):956-62. doi: 10.1021/ja408682s. Epub 2014 Jan 8.

Abstract

Surface-bound polypeptides and proteins are increasingly used to functionalize inorganic interfaces such as electrodes, but their structural characterization is exceedingly difficult with standard technologies. In this paper, we report the first two-dimensional sum-frequency generation (2D SFG) spectra of a peptide monolayer, which are collected by adding a mid-IR pulse shaper to a standard femtosecond SFG spectrometer. On a gold surface, standard FTIR spectroscopy is inconclusive about the peptide structure because of solvation-induced frequency shifts, but the 2D line shapes, anharmonic shifts, and lifetimes obtained from 2D SFG reveal that the peptide is largely α-helical and upright. Random coil residues are also observed, which do not themselves appear in SFG spectra due to their isotropic structural distribution, but which still absorb infrared light and so can be detected by cross-peaks in 2D SFG spectra. We discuss these results in the context of peptide design. Because of the similar way in which the spectra are collected, these 2D SFG spectra can be directly compared to 2D IR spectra, thereby enabling structural interpretations of surface-bound peptides and biomolecules based on the well-studied structure/2D IR spectra relationships established from soluble proteins.

摘要

表面结合的多肽和蛋白质越来越多地用于使诸如电极等无机界面功能化,但其结构表征采用标准技术极为困难。在本文中,我们报告了肽单层的首个二维和频产生(2D SFG)光谱,该光谱是通过在标准飞秒SFG光谱仪上添加一个中红外脉冲整形器来收集的。在金表面,由于溶剂化引起的频率偏移,标准傅里叶变换红外光谱(FTIR)对肽结构的判断并不明确,但从2D SFG获得的二维线形、非谐频移和寿命表明,该肽主要呈α螺旋且垂直排列。还观察到了无规卷曲残基,由于其各向同性的结构分布,它们本身不会出现在SFG光谱中,但它们仍会吸收红外光,因此可以通过2D SFG光谱中的交叉峰检测到。我们在肽设计的背景下讨论了这些结果。由于光谱的收集方式相似,这些2D SFG光谱可以直接与二维红外光谱(2D IR)进行比较,从而能够基于从可溶性蛋白质建立的经过充分研究的结构/二维红外光谱关系,对表面结合的肽和生物分子进行结构解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/078c/3956615/c644ed5eb3f2/nihms554485f1.jpg

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