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α-螺旋抗冻肽在特定冰晶表面平面上的吸附

Adsorption of alpha-helical antifreeze peptides on specific ice crystal surface planes.

作者信息

Knight C A, Cheng C C, DeVries A L

机构信息

National Center for Atmospheric Research, Boulder, Colorado 80307.

出版信息

Biophys J. 1991 Feb;59(2):409-18. doi: 10.1016/S0006-3495(91)82234-2.

DOI:10.1016/S0006-3495(91)82234-2
PMID:2009357
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1281157/
Abstract

The noncolligative peptide and glycopeptide antifreezes found in some cold-water fish act by binding to the ice surface and preventing crystal growth, not by altering the equilibrium freezing point of the water. A simple crystal growth and etching technique allows determination of the crystallographic planes where the binding occurs. In the case of elongated molecules, such as the alpha-helical peptides in this report, it also allows a deduction of the molecular alignment on the ice surface. The structurally similar antifreeze peptides from winter flounder (Pseudopleuronectes americanus) and Alaskan plaice (Pleuronectes quadritaberulatus) adsorb onto the (2021) pyramidal planes of ice, whereas the sculpin (Myoxocephalus scorpius) peptide adsorbs on (2110), the secondary prism planes. All three are probably aligned along (0112). These antifreeze peptides have 11-amino acid sequence repeats ending with a polar residue, and each repeat constitutes a distance of 16.5 A along the helix, which nearly matches the 16.7 A repeat spacing along (0112) in ice. This structural match is undoubtedly important, but the mechanism of binding is not yet clear. The suggested mechanism of growth inhibition operates through the influence of local surface curvature upon melting point and results in complete inhibition of the crystal growth even though individual antifreeze molecules bind at only one interface orientation.

摘要

在一些冷水鱼中发现的非依数性肽和糖肽抗冻剂,其作用方式是与冰表面结合并阻止晶体生长,而不是改变水的平衡冰点。一种简单的晶体生长和蚀刻技术可以确定发生结合的晶体学平面。对于细长分子,如本报告中的α-螺旋肽,它还可以推断出冰表面的分子排列。来自冬比目鱼(美洲拟庸鲽)和阿拉斯加鲽鱼(四突庸鲽)的结构相似的抗冻肽吸附在冰的(2021)锥面上,而杜父鱼(鲬杜父鱼)肽吸附在(2110),即第二棱柱面上。所有这三种肽可能都沿(0112)排列。这些抗冻肽具有以极性残基结尾的11个氨基酸序列重复,每个重复沿螺旋构成16.5埃的距离,这与冰中沿(0112)的16.7埃重复间距几乎匹配。这种结构匹配无疑很重要,但结合机制尚不清楚。所提出的生长抑制机制是通过局部表面曲率对熔点的影响起作用的,即使单个抗冻分子仅在一个界面取向上结合,也会导致晶体生长完全受到抑制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8681/1281157/ee9e521ac16e/biophysj00118-0154-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8681/1281157/ee9e521ac16e/biophysj00118-0154-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8681/1281157/ee9e521ac16e/biophysj00118-0154-a.jpg

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