Accurate Determination of Interfacial Protein Secondary Structure by Combining Interfacial-Sensitive Amide I and Amide III Spectral Signals

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• 作者：Shuji Ye ; Hongchun Li ; Weilai Yang ; Yi Luo
• 刊名：Journal of the American Chemical Society
• 出版年：2014
• 出版时间：January 29, 2014
• 年：2014
• 卷：136
• 期：4
• 页码：1206-1209
• 全文大小：252K
• ISSN：1520-5126

文摘

Accurate determination of protein structures at the interface is essential to understand the nature of interfacial protein interactions, but it can only be done with a few, very limited experimental methods. Here, we demonstrate for the first time that sum frequency generation vibrational spectroscopy can unambiguously differentiate the interfacial protein secondary structures by combining surface-sensitive amide I and amide III spectral signals. This combination offers a powerful tool to directly distinguish random-coil (disordered) and 伪-helical structures in proteins. From a systematic study on the interactions between several antimicrobial peptides (including LK伪14, mastoparan X, cecropin P1, melittin, and pardaxin) and lipid bilayers, it is found that the spectral profiles of the random-coil and 伪-helical structures are well separated in the amide III spectra, appearing below and above 1260 cm^鈥?, respectively. For the peptides with a straight backbone chain, the strength ratio for the peaks of the random-coil and 伪-helical structures shows a distinct linear relationship with the fraction of the disordered structure deduced from independent NMR experiments reported in the literature. It is revealed that increasing the fraction of negatively charged lipids can induce a conformational change of pardaxin from random-coil to 伪-helical structures. This experimental protocol can be employed for determining the interfacial protein secondary structures and dynamics in situ and in real time without extraneous labels.