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人α-抑制因子重链的糖基化模式

Glycosylation pattern of human inter-alpha-inhibitor heavy chains.

作者信息

Flahaut C, Capon C, Balduyck M, Ricart G, Sautiere P, Mizon J

机构信息

Laboratoire de Biochimie, Faculté de Pharmacie, Université de Lille II, Avenue du Professeur Laguesse, B.P. 83, F-59006 Lille, France.

出版信息

Biochem J. 1998 Aug 1;333 ( Pt 3)(Pt 3):749-56. doi: 10.1042/bj3330749.

Abstract

Human inter-alpha-inhibitor (IalphaI) is a plasma serine-proteinase inhibitor. It consists of three polypeptide chains covalently linked by a glycosaminoglycan chain: a light chain named bikunin carrying the anti-proteinase activity and two heavy chains, H1 and H2, which exhibit specific properties, e.g. they interact with hyaluronan thus stabilizing the extracellular matrix. In this study, using matrix-assisted laser desorption ionization-time-of-flight MS and amino acid sequencing of tryptic peptides, we provide a detailed analysis of the glycosylation pattern of both heavy chains. H1 carries two complex-type N-glycans of predominantly biantennary structure linked to asparagine residues at positions 256 and 559 respectively. In contrast, the oligosaccharides attached to H2 are a complex-type N-glycan in the N-terminal region of the protein (Asn64) and three to four type-1 core-structure O-glycans mono- or di-sialylated, clustered in the C-terminal region. We propose that these O-glycans might function as a recognition signal for the H2 heavy chain. The biological implications of this hypothesis, notably for the biosynthetic pathway of IalphaI, are discussed.

摘要

人α-抑制因子(IαI)是一种血浆丝氨酸蛋白酶抑制剂。它由三条通过糖胺聚糖链共价连接的多肽链组成:一条名为比基尼的轻链具有抗蛋白酶活性,以及两条重链H1和H2,它们具有特定特性,例如它们与透明质酸相互作用从而稳定细胞外基质。在本研究中,我们使用基质辅助激光解吸电离飞行时间质谱和胰蛋白酶肽段的氨基酸测序,对两条重链的糖基化模式进行了详细分析。H1携带两个主要为双天线结构的复合型N-聚糖,分别连接到第256位和第559位的天冬酰胺残基上。相比之下,连接到H2的寡糖是蛋白质N端区域(Asn64)的一个复合型N-聚糖,以及三到四个单唾液酸或双唾液酸化的1型核心结构O-聚糖,聚集在C端区域。我们提出这些O-聚糖可能作为H2重链的识别信号。讨论了这一假设的生物学意义,特别是对IαI生物合成途径的意义。

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