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定量分析附着于调理素化细菌表面的人类补体第三成分:调理素缺陷血清和抗吞噬菌株。

Quantitation of the third component of human complement attached to the surface of opsonized bacteria: opsonin-deficient sera and phagocytosis-resistant strains.

作者信息

Verbrugh H A, van Dijk W C, van Erne M E, Peters R, Peterson P K, Verhoef J

出版信息

Infect Immun. 1979 Dec;26(3):808-14. doi: 10.1128/iai.26.3.808-814.1979.

Abstract

The role of the third component of human complement (C3) in the opsonization of bacteria in nonimmune human sera was evaluated. The amount of C3 that becomes attached to the surface of bacteria upon incubation in serum was measured in a quantitative fluorescent immunoassay using fluorescein-conjugated monospecific antiserum to human C3. The intensity of the fluorescence from opsonized bacteria was found to be directly proportional to the absolute amount of C3 fixed, and this enabled the detection of as few as 300 molecules of bound C3 per bacterium. In normal serum the rate of C3 fixation was closely correlated with an increase in opsonization of the bacteria for human PMNs. Both C3 fixation and opsonization were maximal after 15 min of incubation. C3 fixation was also observed, albeit at a significantly slower rate, in human serum with a nonfunctional classical pathway but an intact alternative complement pathway and in serum deficient in immunoglobulins. Again, the kinetics of C3 fixation correlated with bacterial opsonization. Using a total of 21 strains of several bacterial species, including Staphylococcus aureus and Escherichia coli, encapsulation of bacteria was found to interfere with the process of C3 fixation in normal human serum, rendering these organisms resistant to subsequent phagocytosis by human polymorphonuclear leukocytes.

摘要

评估了人类补体第三成分(C3)在非免疫人血清中对细菌的调理作用。使用与荧光素偶联的抗人C3单特异性抗血清,通过定量荧光免疫测定法测量了血清孵育后附着在细菌表面的C3量。发现调理后细菌发出的荧光强度与固定的C3绝对量成正比,这使得能够检测到每个细菌上低至300个结合的C3分子。在正常血清中,C3固定速率与细菌对人中性粒细胞的调理作用增强密切相关。孵育15分钟后,C3固定和调理作用均达到最大值。在经典途径无功能但替代补体途径完整的人血清以及免疫球蛋白缺乏的血清中,也观察到了C3固定,尽管速率明显较慢。同样,C3固定动力学与细菌调理作用相关。使用包括金黄色葡萄球菌和大肠杆菌在内的几种细菌的总共21个菌株,发现细菌的包膜会干扰正常人血清中的C3固定过程,使这些生物体对随后被人多形核白细胞吞噬具有抗性。

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