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人C3的C3c和C3d片段可结合骨髓瘤IgG1和IgG3蛋白。

C3c and C3d fragments of human C3 bind myeloma IgG1 and IgG3 proteins.

作者信息

Hautanen A, Sarnesto A, Keski-Oja J, Seppälä I

出版信息

Immunol Lett. 1982 Nov;5(5):227-32. doi: 10.1016/0165-2478(82)90104-3.

Abstract

Eight human myeloma proteins, two of each IgG subclass, were studied for binding to solid-phase C3c and C3d by the ELISA technique. Myeloma IgG1 kappa, IgG1 lambda, IgG3 kappa and IgG3 lambda proteins bound to C3c and C3d, while two IgG2 kappa, and two IgG4 kappa proteins failed to show significant binding affinity. The results suggest that like C1q, the stable binding sites of C3, located on the C3c and C3d parts of the molecule, have affinity for IgG subclasses 1 and 3.

摘要

采用酶联免疫吸附测定(ELISA)技术研究了8种人骨髓瘤蛋白(每种IgG亚类各2种)与固相C3c和C3d的结合情况。骨髓瘤IgG1 κ、IgG1 λ、IgG3 κ和IgG3 λ蛋白可与C3c和C3d结合,而2种IgG2 κ蛋白和2种IgG4 κ蛋白未表现出明显的结合亲和力。结果表明,与C1q类似,位于分子C3c和C3d部分的C3稳定结合位点对IgG1和IgG3亚类具有亲和力。

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