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通过芯片分析、糖基化芯片数据和质谱的计算整合来破译蛋白质糖基化。

Deciphering Protein Glycosylation by Computational Integration of On-chip Profiling, Glycan-array Data, and Mass Spectrometry.

机构信息

From the Van Andel Research Institute, 333 Bostwick NE, Grand Rapids, MI 49503.

From the Van Andel Research Institute, 333 Bostwick NE, Grand Rapids, MI 49503.

出版信息

Mol Cell Proteomics. 2019 Jan;18(1):28-40. doi: 10.1074/mcp.RA118.000906. Epub 2018 Sep 26.

DOI:10.1074/mcp.RA118.000906
PMID:30257876
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6317472/
Abstract

The difficulty in uncovering detailed information about protein glycosylation stems from the complexity of glycans and the large amount of material needed for the experiments. Here we report a method that gives information on the isomeric variants of glycans in a format compatible with analyzing low-abundance proteins. On-chip glycan modification and probing (on-chip gmap) uses sequential and parallel rounds of exoglycosidase cleavage and lectin profiling of microspots of proteins, together with algorithms that incorporate glycan-array analyses and information from mass spectrometry, when available, to computationally interpret the data. In tests on control proteins with simple or complex glycosylation, on-chip gmap accurately characterized the relative proportions of core types and terminal features of glycans. Subterminal features (monosaccharides and linkages under a terminal monosaccharide) were accurately probed using a rationally designed sequence of lectin and exoglycosidase incubations. The integration of mass information further improved accuracy in each case. An alternative use of on-chip gmap was to complement the mass spectrometry analysis of detached glycans by specifying the isomers that comprise the glycans identified by mass spectrometry. On-chip gmap provides the potential for detailed studies of glycosylation in a format compatible with clinical specimens or other low-abundance sources.

摘要

揭示蛋白质糖基化详细信息的困难源于聚糖的复杂性和实验所需的大量材料。在这里,我们报告了一种方法,该方法以与分析低丰度蛋白质兼容的格式提供糖型异构体的信息。芯片上糖基化修饰和探测(on-chip gmap)使用顺序和并行的外切糖苷酶切割轮次和微点蛋白质的凝集素分析,以及当有可用的聚糖阵列分析和质谱信息时,可计算解释数据的算法。在对具有简单或复杂糖基化的对照蛋白进行的测试中,on-chip gmap 准确地描述了聚糖核心类型和末端特征的相对比例。使用合理设计的凝集素和外切糖苷酶孵育序列,可以准确探测亚末端特征(末端单糖下的单糖和键)。在每种情况下,质量信息的整合都进一步提高了准确性。on-chip gmap 的另一种用途是通过指定通过质谱鉴定的聚糖所包含的异构体来补充游离聚糖的质谱分析。on-chip gmap 提供了以与临床标本或其他低丰度来源兼容的格式进行详细糖基化研究的潜力。

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