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通过傅里叶变换红外光谱法对在有机溶液和模型生物膜中形成3(10)螺旋、α螺旋和β弯曲带状结构的肽进行研究。

Studies of peptides forming 3(10)- and alpha-helices and beta-bend ribbon structures in organic solution and in model biomembranes by Fourier transform infrared spectroscopy.

作者信息

Kennedy D F, Crisma M, Toniolo C, Chapman D

机构信息

Department of Protein and Molecular Biology, Royal Free Hospital School of Medicine, University of London, United Kingdom.

出版信息

Biochemistry. 1991 Jul 2;30(26):6541-8. doi: 10.1021/bi00240a026.

DOI:10.1021/bi00240a026
PMID:2054352
Abstract

In order to examine the potential correlation between infrared absorption spectra and 3(10)- and alpha-helices and beta-bend ribbon structures, the secondary structures of synthetic peptides known to contain pure 3(10)-helices, mixed 3(10)/alpha-helices, and pure beta-bend ribbon structures, based upon X-ray diffraction and NMR studies, have been investigated by using FTIR spectroscopy incorporating resolution-enhancement techniques. Studies of the peptides known to contain a stable 3(10)-helix in CDCl3 show the main amide I band of fully stable 3(10)-helices occurs at 1666-1662 cm-1. Resolution-enhancement methods revealed small contributions at 1681-1678 and 1646-1644 cm-1, while the amide II band occurs at 1533-1531 cm-1. Peptides known to contain both alpha- and 3(10)-helices in their structure exhibit bands characteristic of both types of conformation. Peptides known to fold into the beta-bend ribbon structure show an amide I band maximum at 1648-1645 cm-1 with the amide II band at 1538-1536 cm-1. Incorporation of these peptides into model membrane structures, e.g., DMPC vesicles, in aqueous buffer sometimes produces changes in the peptide secondary structure. Those peptides which possess a 3(10)-helical structure in CDCl3 solution change the secondary structure in DMPC vesicles to predominantly alpha-helical, plus a contribution from short, unstable 3(10)-helix and/or beta-turns. Those peptides which contain a combination of alpha- and 3(10)-helical structures in CDCl3 solution tend to retain some 3(10)-helical structure within the lipid environment, although the overall H-bonding pattern is altered. Those peptides which form a beta-bend ribbon structure appear to be largely unaffected in the membrane environment.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

为了研究红外吸收光谱与3(10)-螺旋、α-螺旋以及β-转角带状结构之间的潜在相关性,基于X射线衍射和核磁共振研究,已知含有纯3(10)-螺旋、混合3(10)/α-螺旋以及纯β-转角带状结构的合成肽的二级结构,已通过使用结合分辨率增强技术的傅里叶变换红外光谱进行了研究。对已知在CDCl3中含有稳定3(10)-螺旋的肽的研究表明,完全稳定的3(10)-螺旋的主要酰胺I带出现在1666 - 1662 cm-1处。分辨率增强方法揭示在1681 - 1678和1646 - 1644 cm-1处有小的贡献,而酰胺II带出现在1533 - 1531 cm-1处。已知其结构中同时含有α-螺旋和3(10)-螺旋的肽表现出两种构象类型的特征带。已知折叠成β-转角带状结构的肽在1648 - 1645 cm-1处有酰胺I带最大值,酰胺II带出现在1538 - 1536 cm-1处。将这些肽掺入模型膜结构(例如二肉豆蔻酰磷脂酰胆碱囊泡)中,在水性缓冲液中有时会导致肽二级结构的变化。那些在CDCl3溶液中具有3(10)-螺旋结构的肽在二肉豆蔻酰磷脂酰胆碱囊泡中会将二级结构转变为主要是α-螺旋,再加上短的、不稳定的3(10)-螺旋和/或β-转角的贡献。那些在CDCl3溶液中含有α-螺旋和3(10)-螺旋结构组合的肽在脂质环境中倾向于保留一些3(10)-螺旋结构,尽管整体氢键模式发生了改变。那些形成β-转角带状结构的肽在膜环境中似乎基本不受影响。(摘要截取自250字)

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