S 蛋白抑制补体 SC5b-9 复合物内的 C9 聚合。

E R Podack, K T Preissner, H J Müller-Eberhard
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摘要

我们研究了 S 蛋白在 C5b-9 复合物组装过程中对 C9 聚合的影响。利用 SDS 聚丙烯酰胺梯度平板凝胶电泳,管状聚 C9 被定量为分子量为 1.1 至 1.3 X 10(6)的抗 SDS 蛋白。将纯化的 C5b-6、C7、C8 和 C9 以 1:1:1:12 的摩尔比进行培养,可形成聚 C9。向蛋白混合物或预组装的 C5b-7 或 C5b-8 中加入纯化的 S 蛋白,会以剂量依赖的方式阻止聚 C9 的形成,并产生 SC5b-9。在电子显微镜下可以看到,从纯化的蛋白质或在酶联免疫吸附素激活的血清中组装的 SC5b-9 呈楔形结构,长度为 350 至 400 A,宽度为 30 至 250 A,缺乏膜攻击复合物(MAC)图像中的管状聚 C9。使用生物素-S 蛋白和涂有阿维丁的胶体金颗粒,S 蛋白位于楔形 SC5b-9 复合物的宽端。结论是 S 蛋白在 SC5b-9 组装过程中具有双重功能。它阻断了 C5b-7 的膜位点,并抑制了 SC5b-8 聚合 C9。因此,SC5b-9 与 MAC 在结构上的主要区别是缺乏管状聚 C9。
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Inhibition of C9 polymerization within the SC5b-9 complex of complement by S-protein.

The effect of S-protein on the polymerization of C9 during assembly of the C5b-9 complex was examined. Utilizing SDS polyacrylamide gradient slab gel electrophoresis, tubular poly C9 was quantitated as SDS resistant protein of 1.1 to 1.3 X 10(6) molecular weight. Poly C9 formation occurred upon incubation of purified C5b-6, C7, C8 and C9 at molar ratios 1:1:1:12. Addition of purified S-protein to the protein mixture or to preassembled C5b-7 or C5b-8 blocked formation of poly C9 in a dose dependent fashion and gave rise to SC5b-9. SC5b-9 assembled from purified proteins or in zymosan-activated serum was visualized in the electron microscope as a wedge-shaped structure of 350 to 400 A length and 30 to 250 A width which lacked tubular poly C9 seen in images of the membrane attack complex (MAC). Using biotinyl-S-protein and colloidal gold particles coated with avidin, S-protein was located at the wide end of the wedge-like SC5b-9 complex. It is concluded that S-protein has a dual function in SC5b-9 assembly. It blocks the membrane site of C5b-7 and it inhibits C9 polymerization by SC5b-8. Accordingly, the main structural difference between SC5b-9 and the MAC is the lack of tubular poly C9.

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