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血清淀粉样蛋白P成分对半乳糖丙酮酸缩醛的结合特异性。

Binding specificity of serum amyloid P component for the pyruvate acetal of galactose.

作者信息

Hind C R, Collins P M, Renn D, Cook R B, Caspi D, Baltz M L, Pepys M B

出版信息

J Exp Med. 1984 Apr 1;159(4):1058-69. doi: 10.1084/jem.159.4.1058.

Abstract

Serum amyloid P component (SAP) is a normal plasma protein that is of interest because of its presence in amyloid deposits, its presence in normal human glomerular basement membrane, and its stable evolutionary conservation. It has calcium-dependent ligand-binding specificity for amyloid fibrils, fibronectin (Fn), C4-binding protein (C4bp), and agarose. Although the binding to agarose, a linear galactan hydrocolloid derived from some marine algae, is unlikely per se to be related to the physiological function of SAP, it does provide a model system in which to explore the precise ligand requirements of SAP. We report here that the amount of SAP from human, mouse, and plaice (Pleuronectes platessa L.) serum able to bind to agarose from different sources reflect precisely their pyruvate content. Methylation with diazomethane of the carboxyl groups in the pyruvate moiety of agarose completely abolishes SAP binding to agarose. The pyruvate in agarose exists as the 4,6-pyruvate acetal of beta-D-galactopyranose. We have therefore synthesized this galactoside, using a novel procedure, established its structure by analysis of its nuclear magnetic resonance spectra, and shown that it completely inhibits all known calcium-dependent binding reactions of SAP. The R isomer of the cyclic acetal, methyl 4,6-O-(1-carboxyethylidene)-beta-D-galactopyranoside (MO beta DG) was effective at millimolar concentration and was more potent than its noncyclic analogue, while pyruvate, D-galactose, and methyl beta-D-galactopyranoside were without effect. The autologous protein ligands of SAP presumably, therefore express a structural determinant(s) that stereochemically resembles MO beta DG. Availability of this specific, well-characterized, low molecular weight ligand for SAP should facilitate further investigation of the function of SAP and its role in physiological and pathophysiological processes.

摘要

血清淀粉样蛋白P成分(SAP)是一种正常的血浆蛋白,因其存在于淀粉样沉积物中、存在于正常人肾小球基底膜中以及具有稳定的进化保守性而备受关注。它对淀粉样纤维、纤连蛋白(Fn)、C4结合蛋白(C4bp)和琼脂糖具有钙依赖性配体结合特异性。尽管与琼脂糖(一种源自某些海藻的线性半乳聚糖水胶体)的结合本身不太可能与SAP的生理功能相关,但它确实提供了一个模型系统,用于探索SAP精确的配体需求。我们在此报告,来自人、小鼠和鲽鱼(Pleuronectes platessa L.)血清中能够与不同来源琼脂糖结合的SAP量准确反映了它们的丙酮酸含量。用重氮甲烷对琼脂糖丙酮酸部分的羧基进行甲基化完全消除了SAP与琼脂糖的结合。琼脂糖中的丙酮酸以β-D-吡喃半乳糖的4,6-丙酮酸缩醛形式存在。因此,我们使用一种新方法合成了这种半乳糖苷,通过分析其核磁共振光谱确定了其结构,并表明它完全抑制了SAP所有已知的钙依赖性结合反应。环状缩醛的R异构体,4,6-O-(1-羧基亚乙基)-β-D-吡喃半乳糖甲酯(MOβDG)在毫摩尔浓度下有效,并且比其非环状类似物更有效,而丙酮酸、D-半乳糖和β-D-吡喃半乳糖甲酯则无作用。因此,SAP的自体蛋白配体可能表达了一种立体化学上类似于MOβDG的结构决定因素。这种针对SAP的特异性、特征明确的低分子量配体的可用性应有助于进一步研究SAP的功能及其在生理和病理生理过程中的作用。

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