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肽GGXA(X = S、T、Y)的化学磷酸化:不同化学方法的评估

Chemical phosphorylation of the peptides GGXA (X = S, T, Y): an evaluation of different chemical approaches.

作者信息

Hoffmann R, Wachs W O, Berger R G, Kalbitzer H R, Waidelich D, Bayer E, Wagner-Redeker W, Zeppezauer M

机构信息

Department of Biochemistry, University of Saarland, Saarbrücken, Germany.

出版信息

Int J Pept Protein Res. 1995 Jan;45(1):26-34. doi: 10.1111/j.1399-3011.1995.tb01564.x.

DOI:10.1111/j.1399-3011.1995.tb01564.x
PMID:7775006
Abstract

An evaluation was made of the two methods most commonly used for phosphorylation of hydroxyamino acids in peptides, i.e. the tetrazole-catalysed phosphitylation by di-tert-butyl-N,N-diethylphosphoramidite followed by oxidation and the phosphorylation by dibenzylphosphochloridate. As model system the sequence GGXA (X = S, T, Y) was used which represents a random-coil sequence avoiding the influence on the reaction kinetics of secondary structure formation. In the case of serine- and threonine-containing peptides, both synthetic methods gave comparable yields of the desired phosphopeptides. The phosphorylation of tyrosine was achieved more favorably via the phosphoramidite method. However, phosphotyrosine peptides are most easily obtained by peptide synthesis using Fmoc-Tyr(PO3Me2)OH as building block. The dibenzylphosphochloridate method yields the expected phosphopeptides as the only peptide derivative and in addition, a great number of unidentified by-products which can be removed by ion-exchange chromatography. The phosphoramidite method consistently resulted in three peptide derivatives, i.e. the desired phosphopeptide, the phosphitylated peptide and a bridged derivative with two GGXA fragments linked through a phosphodiester bridge. The derivatives were characterised by RP and ion-exchange chromatography, 31P- and 1H-NMR spectroscopy, and ion-spray and electrospray mass spectrometry. Interestingly, even these mild ionisation techniques resulted in partial fragmentation. The observed fragmentation pathways seem to be a diagnostic tool for the identification of phosphorylation sites in peptides. Both the phosphorylated serine and threonine peptide lost phosphoric acid (98 mass units), the tyrosine peptide lost phenyl phosphate (174 mass units).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

对肽中羟基氨基酸磷酸化最常用的两种方法进行了评估,即二叔丁基 - N,N - 二乙基磷酰胺在四唑催化下进行磷酰化,随后氧化,以及二苄基磷酰氯进行磷酸化。以序列GGXA(X = S、T、Y)作为模型系统,该序列代表一种无规卷曲序列,避免了二级结构形成对反应动力学的影响。对于含丝氨酸和苏氨酸的肽,两种合成方法得到的所需磷酸肽产率相当。通过磷酰胺方法更有利于实现酪氨酸的磷酸化。然而,磷酸酪氨酸肽最容易通过使用Fmoc - Tyr(PO3Me2)OH作为构建块进行肽合成获得。二苄基磷酰氯方法产生预期的磷酸肽作为唯一的肽衍生物,此外,还有大量未鉴定的副产物,可通过离子交换色谱法去除。磷酰胺方法始终产生三种肽衍生物,即所需的磷酸肽、磷酰化肽和一种通过磷酸二酯桥连接两个GGXA片段的桥连衍生物。通过反相和离子交换色谱法、31P - 和1H - NMR光谱以及离子喷雾和电喷雾质谱对衍生物进行了表征。有趣的是,即使这些温和的电离技术也导致了部分碎片化。观察到的碎片化途径似乎是鉴定肽中磷酸化位点的诊断工具。磷酸化的丝氨酸和苏氨酸肽都失去了磷酸(98质量单位),酪氨酸肽失去了苯磷酸(174质量单位)。(摘要截断于250字)

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