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The effect of complement on the ingestion of soluble antigen-antibody complexes and IgM aggregates by mouse peritoneal macrophages

机译:补体对小鼠腹膜巨噬细胞摄入可溶性抗原-抗体复合物和IgM聚集体的影响

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摘要

Complement was found to stimulate markedly the ingestion of soluble antigen-antibody complexes by mouse peritoneal macrophages. This was shown indirectly by measuring the release of degradation products when the complexes were labeled with 125I, or directly when the antigen, that was human transferrin, was labeled with 59Fe. In this case, the metal which was released from human transferrin inside the cells was not excreted, and its accumulation in the macrophages was a direct index of the uptake of immune complexes. The decay of radioactivity in macrophages after ingestion of 125I-labeled complexes was similar when they were taken up with or without complement, indicating that complement acts primarily on ingestion and not on digestion or excretion. The ingestion of complexes was morphologically confirmed using fluorescein-labeled antigen in the immune complexes. The opsonic effect of complement was also observed with IgM aggregates indicating that soluble complexes can be ingested through complement receptors without involvement of Fc-receptors, as required for particulate antigen-antibody complexes.
机译:发现补体显着刺激小鼠腹膜巨噬细胞对可溶性抗原-抗体复合物的摄取。当用125 I标记复合物时,或者通过用59Fe标记抗原(即人类运铁蛋白)时,直接通过测量降解产物的释放来间接表明这一点。在这种情况下,从人转铁蛋白释放的金属不会在细胞内排泄,其在巨噬细胞中的积累是免疫复合物摄取的直接指标。摄取或不摄取补体时,摄入125 I标记的复合物后,巨噬细胞的放射性衰减相似,这表明补体主要作用于摄入而不是消化或排泄。在免疫复合物中使用荧光素标记的抗原在形态上确认了复合物的摄入。还用IgM聚集体观察到补体的调理作用,表明可溶的复合物可以通过补体受体摄取,而无需Fc受体的参与,如颗粒抗原-抗体复合物所要求的。

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