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外文期刊>The journal of immunology
>Cleavage of the Third Complement Component (C3) and Generation of the Spasmogenic Peptide, C3a, in Human Serum Via the Properdin Pathway: Demonstration of Inhibitory As Well As Enhancing Effects of Epsilon-Amino-Caproic Acid
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Cleavage of the Third Complement Component (C3) and Generation of the Spasmogenic Peptide, C3a, in Human Serum Via the Properdin Pathway: Demonstration of Inhibitory As Well As Enhancing Effects of Epsilon-Amino-Caproic Acid
Human and guinea pig serum loses hemolytic activity of the third complement component (C3) during incubation at 37°C. The loss is due to specific C3 cleavage involving the properdin system. This is concluded from the finding that C3 inactivation is prevented by EDTA, by elimination of properdin factor B, and unimpaired in C4 deficient guinea pig serum.In the presence of 1 M ε-amino-caproic acid (EACA) spontaneous C3 cleavage is considerably enhanced and accompanied by the appearance of biologically active C3a. Lower concentrations of EACA inhibit rather than enhance C3 cleavage in serum. The inhibitory effect of EACA is due to interference with the interaction of the properdin factors and their action on C3 as demonstrated in various systems: the assembly of an active C3-cleaving complex on zymosan, its regeneration after decay by factor D and factor B (GBG), cleavage of GBG by C3b and factor D in systems of purified components, and cleavage of C3 by preformed properdin complexes. Reactions involving the cobra venom factor were likewise depressed. In all these systems EACA was inhibitory even at 1 M concentration. No single step in the development or action of an active properdin system was found to be enhanced by 1 M EACA. The enhancing effect of high concentrations of EACA on C3 cleavage in serum may be explained by its observed inhibition of C3b inactivator (C3bINA). This factor controls the properdin system by destroying C3b. In serum the inhibitory effect of 1 M EACA on C3bINA appears to allow escape of the properdin system from its control and thus to increase its net activity toward C3 despite inhibition of the enzymic reactions proper. At lower concentrations the effect of EACA on C3bINA is apparently less significant; therefore, at low concentrations of EACA, its inhibitory effects on C3 cleavage by the properdin system in serum predominate.
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机译:人和豚鼠血清在37°C孵育期间丧失了第三补体成分(C3)的溶血活性。损失是由于涉及备解素系统的特定C3裂解。结论是EDTA阻止了C3的灭活,消除了备解素因子B并在C4缺乏的豚鼠血清中没有受损。在存在1 Mε-氨基己酸(EACA)的情况下,C3的自发裂解相当可观增强并伴有生物活性C3a的出现。较低浓度的EACA抑制而不是增强血清中C3的裂解。 EACA的抑制作用是由于干扰备解素因子的相互作用及其对C3的作用,如在各种系统中所示:在酵母聚糖上组装有活性的C3裂解复合物,其分解后被D和B因子再生( GBG),C3b和因子D在纯化成分的系统中切割GBG,以及预先形成的备解素复合物对C3的切割。涉及眼镜蛇毒因子的反应同样被抑制。在所有这些系统中,EACA甚至在1 M浓度下都具有抑制作用。发现1 M EACA不会增强主动备解素系统的开发或作用的任何一步。高浓度的EACA对血清C3裂解的增强作用可能是由其对C3b灭活剂(C3bINA)的抑制作用所解释的。该因子通过破坏C3b来控制备解素系统。在血清中,1 M EACA对C3bINA的抑制作用似乎使备解素系统脱离了其对照,因此尽管抑制了适当的酶促反应,但仍增加了其对C3的净活性。在较低的浓度下,EACA对C3bINA的作用显然不那么明显;因此,在低浓度的EACA中,其对血清中备解素系统对C3裂解的抑制作用占主导。
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