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首页> 外文期刊>The journal of immunology >Biphasic Effect of Gingipains from Porphyromonas gingivalis on the Human Complement System
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Biphasic Effect of Gingipains from Porphyromonas gingivalis on the Human Complement System

机译:牙龈卟啉单胞菌的银杏苷对人补体系统的两相作用

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Periodontitis is an inflammatory disease of the supporting structures of the teeth and is caused by, among other agents, Porphyromonas gingivalis . P. gingivalis is very resistant to killing by human complement, which is present in a gingival fluid at 70% of the serum concentration. We found that the incubation of human serum with purified cysteine proteases of P. gingivalis (gingipains) or P. gingivalis wild-type strains W83 and W50 resulted in a drastic decrease of the bactericidal activity of the serum. In contrast, serum treated with P. gingivalis mutants lacking gingipains (particularly strains without HRgpA) maintained significant bactericidal activity. To understand in detail the mechanism by which gingipains destroy the serum bactericidal activity, we investigated the effects of gingipains on the human complement system. We found that all three proteases degraded multiple complement components, with arginine-specific gingipains (HRgpA and RgpB) being more efficient than lysine-specific gingipain (Kgp). Interestingly, all three proteases at certain concentrations were able to activate the C1 complex in serum, which resulted in the deposition of C1q on inert surfaces and on bacteria themselves. It is therefore plausible that P. gingivalis activates complement when present at low numbers, resulting in a local inflammatory reaction and providing the bacteria with a colonization opportunity and nutrients. At later stages of infection the concentration of proteases is high enough to destroy complement factors and thus render the bacteria resistant to the bactericidal activity of complement.
机译:牙周炎是牙齿支撑结构的炎性疾病,除其他因素外,还由牙龈卟啉单胞菌引起。牙龈卟啉单胞菌对人补体具有很高的抵抗力,人补体以血清浓度的70%存在于牙龈液中。我们发现人血清与齿龈假单胞菌(gingipains)或齿龈假单胞菌野生型菌株W83和W50的纯化的半胱氨酸蛋白酶的孵育导致血清杀菌活性的急剧降低。相比之下,用缺乏牙龈蛋白酶的牙龈卟啉单胞菌突变体(特别是没有HRgpA的菌株)治疗的血清仍具有显着的杀菌活性。为了详细了解姜黄素破坏血清杀菌活性的机理,我们研究了姜黄素对人补体系统的影响。我们发现,所有三种蛋白酶都降解了多种补体成分,其中精氨酸特异性姜黄素(HRgpA和RgpB)比赖氨酸特异性姜黄素(Kgp)更有效。有趣的是,所有三种蛋白酶在一定浓度下都能够激活血清中的C1复合物,从而导致C1q沉积在惰性表面和细菌自身上。因此,当牙龈卟啉单胞菌数量少时,它可能激活补体,导致局部炎症反应,并为细菌提供定植的机会和营养。在感染的后期阶段,蛋白酶的浓度足够高以破坏补体因子,从而使细菌对补体的杀菌活性具有抗性。

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