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短杆菌肽S:一种用于蛋白质糖基化及利用亲核胺逆转糖基化的肽模型。

Gramicidin S: a peptide model for protein glycation and reversal of glycation using nucleophilic amines.

作者信息

Shakkottai V G, Sudha R, Balaram P

机构信息

Molecular Biophysics Unit, Indian Institute of Science, Bangalore, India.

出版信息

J Pept Res. 2002 Aug;60(2):112-20. doi: 10.1034/j.1399-3011.2002.02901.x.

DOI:10.1034/j.1399-3011.2002.02901.x
PMID:12102724
Abstract

Nonenzymatic glycation of proteins has been implicated in various diabetic complications and age-related disorders. Proteins undergo glycation at the N-terminus or at the epsilon-amino group of lysine residues. Glycation of proteins proceeds through the stages of Schiff base formation, conversion to ketoamine product and advanced glycation end products. Gramicidin S, which has two ornithine residues, was used as a model system to study the various stages of glycation of proteins using electrospray ionization mass spectrometry. The proximity of two ornithine residues in the peptide favors the glycation reaction. Formation of advanced glycation end products and diglycation on ornithine residues in gramicidin S were observed. The formation of Schiff base adduct is reversible, whereas the Amadori rearrangement to the ketoamine product is irreversible. Nucleophilic amines and hydrazines can deglycate the Schiff base adduct of glucose with peptides and proteins. Hydroxylamine, isonicotinic acid hydrazide and aminoguanidine effectively removed glucose from the Schiff base adduct of gramicidin S. Hydroxylamine is more effective in deglycating the adduct compared with isonicotinic acid hydrazide and aminoguanidine. The observation that the hydrazines are effective in deglycating the Schiff base adduct even in the presence of high concentrations of glucose, may have a possible therapeutic application in preventing complications of diabetes mellitus. Hydrazines may be used to distinguish between the Schiff base and the ketoamine products formed at the initial stages of glycation.

摘要

蛋白质的非酶糖基化与多种糖尿病并发症及年龄相关疾病有关。蛋白质在N端或赖氨酸残基的ε-氨基处发生糖基化。蛋白质糖基化过程包括席夫碱形成、转化为酮胺产物以及晚期糖基化终产物等阶段。短杆菌肽S含有两个鸟氨酸残基,被用作模型系统,通过电喷雾电离质谱法研究蛋白质糖基化的各个阶段。肽中两个鸟氨酸残基的 proximity 有利于糖基化反应。观察到短杆菌肽S中鸟氨酸残基上晚期糖基化终产物的形成和双糖基化。席夫碱加合物的形成是可逆的,而向酮胺产物的阿马多里重排是不可逆的。亲核胺和肼可以使葡萄糖与肽和蛋白质形成的席夫碱加合物脱糖基化。羟胺、异烟肼和氨基胍能有效地从短杆菌肽S的席夫碱加合物中去除葡萄糖。与异烟肼和氨基胍相比,羟胺在使加合物脱糖基化方面更有效。即使在高浓度葡萄糖存在的情况下,肼能有效地使席夫碱加合物脱糖基化这一观察结果,可能在预防糖尿病并发症方面有潜在的治疗应用。肼可用于区分糖基化初始阶段形成的席夫碱和酮胺产物。

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