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ATP耗竭前后自体IgG与人红细胞的结合。无血影蛋白囊泡上结合位点(自身抗原)的选择性暴露。

Binding of autologous IgG to human red blood cells before and after ATP-depletion. Selective exposure of binding sites (autoantigens) on spectrin-free vesicles.

作者信息

Müller H, Lutz H U

出版信息

Biochim Biophys Acta. 1983 Apr 6;729(2):249-57. doi: 10.1016/0005-2736(83)90491-1.

Abstract

Binding of autologous IgG to fresh, ATP-depleted red blood cells as well as to spectrin-free vesicles was studied by a non-equilibrium binding assay using 125I-iodinated protein A from Staphylococcus aureus. IgG binding was 14-times higher to spectrin-free vesicles than to ATP-maintaining red blood cells and 4-times higher than to ATP-depleted erythrocytes from which these vesicles were released. Protein A binding to vesicles that were released from washed and nutrient-deprived erythrocytes, was dependent on added autologous IgG. However, spectrin-free vesicles that were spontaneously released from erythrocytes conserved in whole blood, bound similar amounts of protein A with or without added autologous IgG (0.45-0.55 ng/micrograms band 3 protein). These findings demonstrate that opsonization of spectrin-free vesicles by autologous IgG occurs not only in the test tube, but also under blood blank conditions. The binding characteristics of IgG to spectrin-free vesicles are indicative of a natural autoantibody rather than an unspecific binding of autologous IgG. The preferential binding of IgG to spectrin-free vesicles implies a selective exposure of corresponding autoantigens in membrane regions that have lost cytoskeletal anchorage and bud off.

摘要

利用来自金黄色葡萄球菌的125I-碘化蛋白A,通过非平衡结合试验研究了自体IgG与新鲜的、ATP耗尽的红细胞以及无血影蛋白囊泡的结合情况。与维持ATP的红细胞相比,IgG与无血影蛋白囊泡的结合高14倍,比释放出这些囊泡的ATP耗尽的红细胞高4倍。蛋白A与从洗涤过的、营养缺乏的红细胞释放出的囊泡的结合,依赖于添加的自体IgG。然而,从全血中保存的红细胞自发释放出的无血影蛋白囊泡,无论是否添加自体IgG,结合的蛋白A量相似(每微克带3蛋白0.45 - 0.55纳克)。这些发现表明,自体IgG对无血影蛋白囊泡的调理作用不仅发生在试管中,也发生在血液空白条件下。IgG与无血影蛋白囊泡的结合特性表明是一种天然自身抗体,而非自体IgG的非特异性结合。IgG对无血影蛋白囊泡的优先结合意味着在失去细胞骨架锚定并芽生的膜区域中,相应自身抗原的选择性暴露。

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