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从人补体的第三和第五成分中衍生出两种不同的过敏毒素活性。

The derivation of two distinct anaphylatoxin activities from the third and fifth components of human complement.

作者信息

Cochrane C G, Müller-Eberhard H J

出版信息

J Exp Med. 1968 Feb 1;127(2):371-86. doi: 10.1084/jem.127.2.371.

Abstract

Anaphylatoxin activity was derived from both human C'5 and C'3 molecules. This was achieved in the case of C'5 by interaction with trypsin or with EAC'4, (oxy)2a, 3. The smooth muscle-contracting material obtained from the treated C'5 was found to be a fragment of approximately 9,000-11,000 molecular weight. Its action was inhibited with antihistamine. The trypsinized C'5 also increased vascular permeability in guinea pig skin. When human C'3 was incubated with C'3 inactivator complex, which consists of a cobra venom protein and a beta-globulin of human serum, anaphylatoxin activity was observed. The activity was associated with a fragment cleaved from the C'3 molecule, having a molecular weight of between 6,000 and 15,000 as determined by gel filtration techniques. Similar activity was derived from C'3 by the C'3-converting enzyme in free or in cell-bound form. The C'5 anaphylatoxin failed to cross-desensitize guinea pig ileum to the contracting capacities of C'3 and guinea pig anaphylatoxin and vice versa. Anaphylatoxin prepared from C'3 by all methods mentioned above caused cross-desensitization to the other C'3 derivatives, but failed to desensitize to guinea pig anaphylatoxin.

摘要

过敏毒素活性源自人补体C5和C3分子。对于C5而言,通过与胰蛋白酶或EAC'4、(oxy)2a、3相互作用可实现这一点。从经处理的C5中获得的平滑肌收缩物质被发现是一种分子量约为9000 - 11000的片段。其作用可被抗组胺药抑制。经胰蛋白酶处理的C5还可增加豚鼠皮肤的血管通透性。当人C3与由眼镜蛇毒蛋白和人血清β球蛋白组成的C3灭活剂复合物一起孵育时,可观察到过敏毒素活性。该活性与从C3分子裂解出的一个片段相关,通过凝胶过滤技术测定其分子量在6000至15000之间。游离或结合于细胞的C3转化酶也可从C3产生类似活性。C5过敏毒素不能使豚鼠回肠对C3和豚鼠过敏毒素的收缩能力产生交叉脱敏,反之亦然。通过上述所有方法从C3制备的过敏毒素会对其他C3衍生物产生交叉脱敏,但对豚鼠过敏毒素则无脱敏作用。

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[ON THE NATURE OF ANAPHYLATOXIN].[关于过敏毒素的性质]
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