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用乙二醇四乙酸和氯化镁 - 乙二醇四乙酸处理的人血清中补体经典途径和替代途径的功能

Function of the classical and alternate pathways of human complement in serum treated with ethylene glycol tetraacetic acid and MgCl2-ethylene glycol tetraacetic acid.

作者信息

Des Prez R M, Bryan C S, Hawiger J, Colley D G

出版信息

Infect Immun. 1975 Jun;11(6):1235-43. doi: 10.1128/iai.11.6.1235-1243.1975.

Abstract

An immunochemical and functional analysis of the classical and alternate complement pathways in human serum was performed in the presence of 10 mM ethylene glycol tetraacetic acid (EGTA) and MgCl(2)-EGTA (MgEGTA), chelating agents which have been recently utilized as a means of distinguishing between these two complement pathways. Total hemolytic activity, integrity of the C1 complex, hemolytic activity of C2, conversion of factor B (C3 proactivator), and complement-dependent bactericidal activity were studied. The effect of these chelators on activation of complement pathways by Escherichia coli, by sensitized erythrocytes as a prototype of activators of the classical pathway, and by zymosan as a prototype of alternate (properdin) pathway activators was studied. Human serum containing 10 mM EGTA, which provides almost no ionized calcium and considerably less ionized magnesium than unchelated serum, allowed consumption of complement via the alternate (properdin) pathway, but blocked the classical pathway as judged by disintegration of the C1 complex and lack of utilization of C2. However, activity of the alternate complement pathway in EGTA serum, as judged by conversion of factor B and bactericidal activity against gram-negative bacteria, was distinctly suboptimal. Addition of magnesium ion in a concentration equimolar to EGTA (MgEGTA serum), while still providing conditions in which the C1 complex dissociated, significantly enhanced alternate complement pathway-mediated bactericidal activity. However, in MgEGTA serum considerable fluid-phase activation of the alternate pathway, as indicated by decrease in 50% hemolytic complement (CH(5 0)) titers and conversion of factor B to its active form in the absence of any activating challenge, was observed. Moreover, some fluid-phase consumption of C2 was observed in MgEGTA serum, even though, as mentioned, the C1 complex was shown to be dissociated under these conditions. MgEGTA-related activation of C2 and of the alternate (properdin) pathway of complement was significantly enhanced by the presence of zymosan and E. coli. These results indicate that use of the chelating agents EGTA and MgEGTA to differentiate between classical and alternate pathway activation of human complement is more complex than has hitherto been suggested. In EGTA serum, spontaneous activation of either pathway does not occur but bactericidal activity, as a measure of biologic function of complement, is suboptimal. In MgEGTA serum, bactericidal activity is fully expressed, but there is considerable instability, in terms of fluid-phase activation, in Mg(2+)-dependent components of both pathways. Thus, caution is indicated in the use and interpretation of the effects of these chelating agents on biologic functions mediated by either pathway of human complement.

摘要

在10 mM乙二醇四乙酸(EGTA)和氯化镁-EGTA(MgEGTA)存在的情况下,对人血清中的经典补体途径和替代补体途径进行了免疫化学和功能分析。这两种螯合剂最近被用作区分这两种补体途径的手段。研究了总溶血活性、C1复合物的完整性、C2的溶血活性、B因子(C3前激活剂)的转化以及补体依赖性杀菌活性。研究了这些螯合剂对大肠杆菌、作为经典途径激活剂原型的致敏红细胞以及作为替代(备解素)途径激活剂原型的酵母聚糖激活补体途径的影响。含有10 mM EGTA的人血清,其提供的游离钙几乎为零,游离镁比未螯合的血清少得多,允许通过替代(备解素)途径消耗补体,但通过C1复合物的解体和C2未被利用判断其阻断了经典途径。然而,通过B因子的转化和对革兰氏阴性菌的杀菌活性判断,EGTA血清中替代补体途径的活性明显次优。添加与EGTA等摩尔浓度的镁离子(MgEGTA血清),虽然仍提供C1复合物解离的条件,但显著增强了替代补体途径介导的杀菌活性。然而,在MgEGTA血清中,观察到替代途径有相当程度的液相激活,表现为50%溶血补体(CH50)滴度降低以及在没有任何激活刺激的情况下B因子转化为其活性形式。此外,在MgEGTA血清中观察到C2有一些液相消耗,尽管如前所述,在这些条件下C1复合物被证明是解离的。酵母聚糖和大肠杆菌的存在显著增强了MgEGTA相关的C2激活以及补体的替代(备解素)途径。这些结果表明,使用螯合剂EGTA和MgEGTA来区分人补体经典途径和替代途径的激活比迄今所认为的更为复杂。在EGTA血清中,两条途径均不会自发激活,但作为补体生物学功能指标的杀菌活性次优。在MgEGTA血清中,杀菌活性充分表达,但就液相激活而言,两条途径中依赖镁离子的成分都有相当大的不稳定性。因此,在使用和解释这些螯合剂对人补体任一途径介导的生物学功能的影响时需谨慎。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b5c2/415205/fe6de0810408/iai00234-0076-a.jpg

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