冻融激活补体攻击期:2。C—56转化酶与冻融法生成的C—56的比较。

A Dessauer, U Rother, K Rother
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引用次数: 0

摘要

c攻击阶段的激活不一定涉及C5转换酶的组成部分。C- 56溶血活性是由同一来源的C7缺失血清通过替代途径转化酶或冷冻和解冻产生的。与转化酶激活相比,冷冻激活后C5a的生物活性(趋化性、血清素释放)未被检测到。C—56溶血活性的产率相似,活性产物的性质相同。在分子量、疏水性和电荷方面没有发现差异。在C7不存在时,这两种活性在37℃时稳定,在C7存在时,这两种活性迅速衰减。本文提出,分子三级结构的构象变化是形成活性C- 56配合物的关键事件。从这个角度来看,转化酶将C5a从天然分子中切割出来似乎是一个副反应,而不是激活所必需的。
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Freeze-thaw activation of the complement attack phase: II. Comparison of convertase generated C--56 with C--56 generated by freezing and thawing.

The activation of the C-attack phase does not necessarily involve the components of the C5 convertases. C--56 hemolytic activity was generated from the same source of C7 depleted serum by the alternative pathway convertase or by freezing and thawing resp. In contrast to activation by the convertase, biological activities of C5a (chemotaxis, serotonin release) were not detected following activation by freezing. The yields of C--56 hemolytic activities were similar and the properties of the activated products were identical. No difference was found in the molecular weight, in the hydrophobicity or with respect to charge. The two activities were in the absence of C7 stable at 37 degrees C and decayed rapidly in the presence of C7. It is proposed that a conformational change in the tertiary structure of the molecule(s) is the critical event in the formation of an active C--56 complex. In this light the cleavage of C5a from the native molecule by the convertase appears as a side reaction, not by itself essential for activation.

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