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质谱法在人类遗传性N-糖基化缺陷特征分析中的应用

Mass spectrometry in the characterization of human genetic N-glycosylation defects.

作者信息

Barone Rita, Sturiale Luisa, Garozzo Domenico

机构信息

Institute of Chemistry and Technology of Polymers, CNR, Catania, Italy.

出版信息

Mass Spectrom Rev. 2009 May-Jun;28(3):517-42. doi: 10.1002/mas.20201.

Abstract

Human genetic diseases that affect N-glycosylation result from the defective synthesis of the N-linked sugar moiety (glycan) of glycoproteins. The role of glycans for proper protein folding and biological functions is illustrated in the variety and severity of clinical manifestations shared by congenital disorders of glycosylation (CDG). This family of inherited metabolic disorders includes defects in the assembly of the oligosaccharide precursor that lead to an under-occupancy of N-glycosylation sites (CDG-I), and defects of glycan remodeling (CDG-II). Mass spectrometry constitutes a key tool for characterization of CDG-I defects by mass resolution of native protein glycoforms that differ for glycosylation-site occupancy. Glycan MS analyses in CDG-II is mandatory to detect whenever possible a repertoire of structures to pinpoint candidate enzymes and genes responsible for the abnormal N-glycan synthesis. In this manuscript, we review the MS applications in the area of CDG and related disorders with a special emphasis on those techniques that have been already applied or might become functional for diagnosis, characterization, and treatment monitoring in some specific conditions.

摘要

影响N-糖基化的人类遗传疾病是由糖蛋白的N-连接糖部分(聚糖)合成缺陷引起的。先天性糖基化障碍(CDG)所共有的各种临床表现及其严重程度,说明了聚糖在蛋白质正确折叠和生物学功能中的作用。这一遗传性代谢疾病家族包括寡糖前体组装缺陷导致N-糖基化位点占用不足的疾病(CDG-I),以及聚糖重塑缺陷的疾病(CDG-II)。质谱分析是通过对因糖基化位点占用不同而不同的天然蛋白质糖型进行质量分辨来表征CDG-I缺陷的关键工具。CDG-II中的聚糖质谱分析对于尽可能检测出一系列结构以确定负责异常N-聚糖合成的候选酶和基因是必不可少的。在本手稿中,我们综述了质谱在CDG及相关疾病领域的应用,特别强调了那些已经应用或可能在某些特定条件下用于诊断、表征和治疗监测的技术。

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