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糖蛋白及其与人类疾病的关系。

Glycoproteins and their relationship to human disease.

作者信息

Brockhausen I, Schutzbach J, Kuhns W

机构信息

Biochemistry Department, University of Toronto, and The Terrence Donnelly Heart Centre, St. Michael's Hospital, Toronto, Canada.

出版信息

Acta Anat (Basel). 1998;161(1-4):36-78. doi: 10.1159/000046450.

Abstract

Glycoproteins are proteins that carry N- and O-glycosidically-linked carbohydrate chains of complex structures and functions. N-glycan chains are assembled in the endoplasmic reticulum and the Golgi by a controlled sequence of glycosyltransferase and glycosidase processing reactions involving dolichol intermediates. The assembly of O-glycans occurs in the Golgi and does not involve dolichol. For most reactions, families of glycosyltransferases exist; the expression of the individual enzymes within a family is often subject to complex regulation. The biosynthesis of N- and O-glycan is controlled at the level of gene expression, mRNA, enzyme protein activity and localization, and through substrate and cofactor concentrations at the site of synthesis. This complex regulation results in many hundreds of structures, the range of which varies in different species, cell types, tissue types, states of development and differentiation. In diseased cells, the relative proportions of these structures are often characteristically different from normal, and may be useful for the assessment of the stage of the disease and for diagnosis. Knowledge of disease-specific glycoprotein structures and their functions may be used therapeutically, in immunotherapy, in blocking cell adhesion or interfering with other binding or biological processes. Recently, some of the mechanisms underlying glycoprotein alterations in disease have been elucidated. This opens the possibility of an active interference in the disease process. The functions of glycans in diseased cells will become more clear with the tools of molecular biology and transgenic animal models.

摘要

糖蛋白是一类带有通过N-糖苷键和O-糖苷键连接的具有复杂结构和功能的碳水化合物链的蛋白质。N-聚糖链在内质网和高尔基体中通过一系列由糖基转移酶和糖苷酶参与的、涉及多萜醇中间体的加工反应按受控顺序组装而成。O-聚糖的组装发生在高尔基体中,且不涉及多萜醇。对于大多数反应而言,存在糖基转移酶家族;一个家族中各个酶的表达通常受到复杂的调控。N-聚糖和O-聚糖的生物合成在基因表达、mRNA、酶蛋白活性和定位水平上受到控制,并通过合成位点处的底物和辅因子浓度进行调控。这种复杂的调控导致了数百种结构的产生,其范围在不同物种、细胞类型、组织类型、发育和分化状态中有所不同。在患病细胞中,这些结构的相对比例通常与正常情况有显著差异,可能有助于评估疾病阶段和进行诊断。对疾病特异性糖蛋白结构及其功能的了解可用于治疗,如免疫治疗、阻断细胞黏附或干扰其他结合或生物学过程。最近,一些疾病中糖蛋白改变的潜在机制已被阐明。这为积极干预疾病进程提供了可能性。随着分子生物学工具和转基因动物模型的应用,患病细胞中聚糖的功能将变得更加清晰。

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