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人C反应蛋白的凝集素特异性与结合特性

Lectin specificity and binding characteristics of human C-reactive protein.

作者信息

Köttgen E, Hell B, Kage A, Tauber R

机构信息

Institut für Klinische Chemie und Biochemie, Universitätsklinikum Rudolf Virchow, Freie Universität Berlin, FRG.

出版信息

J Immunol. 1992 Jul 15;149(2):445-53.

PMID:1624792
Abstract

C-reactive protein (CRP) is thought to play an important role in immunomodulation. The exact biologic function of this pentraxin protein is, however, still unclear. Here we report experiments designed to further characterize the binding properties of CRP. Using purified human CRP it could be shown that CRP immobilized onto polystyrene surfaces or onto latex beads binds distinct plasma glycoproteins including IgG, asialofetuin, asialo-beta 2-glycoprotein I and, likewise, synthetic glycoproteins as a lectin, exhibiting binding specificity for terminal galactosyl residues of the glycoprotein glycans. Binding of CRP to IgA, IgM, IgG, asialofetuin, asialo-beta 2-glycoprotein I and to synthetic glycoproteins requires immobilization onto surfaces of both CRP and the ligand. Fibronectin and fibrinogen are bound by surface-immobilized CRP also in soluble phase. Comparing various mono-, di-, and trisaccharides as competitive inhibitors of the lectin binding activity of CRP, only beta-D-Gal-(1-3)-D-GalNAc, beta-D-Gal-(1-4)-D-GalNAc, and beta-D-Gal-(1-4)-beta-D-Gal-(1-4)-D-GlcNAc had significant inhibitory power at a concentration of 8 mmol/liter. Binding activity of CRP was pH-dependent with an optimum at pH 5 to 6 and was reduced by 90% when pH was shifted from 6 to the physiologic pH value of 7.4. CRP exhibited lectin-like properties with binding specificity for galactosyl residues also when bound to K-562 erythroleukemia cells. It is therefore suggested that CRP immobilized onto surfaces exhibits lectin activity toward galactosyl groups preferentially in a mildly acidic environment as present at sites of inflammation.

摘要

C反应蛋白(CRP)被认为在免疫调节中发挥重要作用。然而,这种五聚体蛋白的确切生物学功能仍不清楚。在此,我们报告旨在进一步表征CRP结合特性的实验。使用纯化的人CRP可以表明,固定在聚苯乙烯表面或乳胶珠上的CRP结合不同的血浆糖蛋白,包括IgG、去唾液酸胎球蛋白、去唾液酸β2-糖蛋白I,同样也结合合成糖蛋白作为凝集素,对糖蛋白聚糖的末端半乳糖基残基表现出结合特异性。CRP与IgA、IgM、IgG、去唾液酸胎球蛋白、去唾液酸β2-糖蛋白I以及合成糖蛋白的结合需要CRP和配体都固定在表面。纤连蛋白和纤维蛋白原也在可溶性相中被表面固定的CRP结合。比较各种单糖、二糖和三糖作为CRP凝集素结合活性的竞争性抑制剂,只有β-D-半乳糖-(1-3)-D- N-乙酰半乳糖胺、β-D-半乳糖-(1-4)-D- N-乙酰半乳糖胺和β-D-半乳糖-(1-4)-β-D-半乳糖-(1-4)-D- N-乙酰葡糖胺在8 mmol/L的浓度下具有显著的抑制能力。CRP的结合活性依赖于pH,在pH 5至6时最佳,当pH从6转变为生理pH值7.4时,活性降低90%。当CRP与K-562红白血病细胞结合时,也表现出对半乳糖基残基的凝集素样特性,具有结合特异性。因此,有人提出,固定在表面的CRP在炎症部位存在的轻度酸性环境中优先对半乳糖基表现出凝集素活性。

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