与免疫复合物相比,c反应蛋白复合物的炎症潜能

Ivan R. Romero , Carol Morris , Monica Rodriguez , Terry W. Du Clos , Carolyn Mold
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引用次数: 15

摘要

c反应蛋白(CRP)是一种急性期血清蛋白,可与磷脂胆碱(PC)和受损组织的成分结合。CRP与抗体相似,它与配体结合并激活经典的补体途径。为了比较CRP复合物和IgG复合物的加工过程,我们制备了含有相同配体的复合物,pc偶联BSA,以及针对BSA或CRP的IgG抗体。我们之前证明了类似的补体介导的这些复合物与红细胞补体受体的结合。CRP和IgG也与中性粒细胞(PMN)上的受体结合,为清除配体提供了另一种可能的途径。PMN结合IgG复合物可导致活化和破坏性炎症后果。在本报告中,我们使用含有PC-BSA的CRP和IgG复合物来比较PMN与内皮细胞的结合和PMN粘附的激活。结果表明,CRP复合物不能激活PMN,而IgG复合物可以。结合试验表明,与CRP复合物相比,IgG复合物与PMN的结合要大得多。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inflammatory Potential of C-Reactive Protein Complexes Compared to Immune Complexes

C-reactive protein (CRP) is an acute phase serum protein that binds to phosphocholine (PC) and to components of damaged tissue. CRP resembles antibody in that it binds to ligands and activates the classical complement pathway. To compare the processing of CRP complexes to that of IgG complexes, we have prepared complexes containing the same ligand, PC-conjugated BSA, and IgG antibody to either BSA or CRP. We previously demonstrated similar complement-mediated binding of these complexes to erythrocyte complement receptors. CRP and IgG also bind to receptors on neutrophils (PMN), providing another possible pathway for clearance of ligands. PMN binding of IgG complexes can lead to activation with damaging inflammatory consequences. In the present report we have used CRP and IgG complexes containing PC-BSA to compare binding to PMN and activation of PMN adherence to endothelial cells. The results indicate that CRP complexes do not activate PMN whereas IgG complexes do. Binding assays indicate that there is substantially greater binding of IgG than CRP complexes to PMN.

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