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Anti-complement activity of the Ixodes scapularis salivary protein Salp20

机译:肩x突唾液蛋白Salp20的抗补体活性

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摘要

Complement, a major component of innate immunity, presents a rapid and robust defense of the intravascular space. While regulatory proteins protect host cells from complement attack, when these measures fail, unrestrained complement activation may trigger self-tissue injury, leading to pathologic conditions. Of the three complement activation pathways, the alternative pathway (AP) in particular has been implicated in numerous disease and injury states. Consequently, the AP components represent attractive targets for therapeutic intervention. The common hard-bodied ticks from the family Ixodidae derive nourishment from the blood of their mammalian hosts. During its blood meal the tick is exposed to host immune effectors, including the complement system. In defense, the tick produces salivary proteins that can inhibit host immune functions. The Salp20 salivary protein of Ixodes scapularis inhibits the host AP pathway by binding properdin and dissociating C3bBbP, the active C3 convertase. In these studies we examined Salp20 activity in various complement-mediated pathologies. Our results indicate that Salp20 can inhibit AP-dependent pathogenesis in the mouse. Its efficacy may be part in due to synergic effects it provides with the endogenous AP regulator, factor H. While Salp20 itself would be expected to be highly immunogenic and therefore inappropriate for therapeutic use, its emergence speaks for the potential development of a non-immunogenic Salp20 mimic that replicates its anti-properdin activity.
机译:补体是先天免疫的主要组成部分,对血管内空间具有快速而强大的防御作用。尽管调节蛋白可以保护宿主细胞免受补体攻击,但是当这些措施失败时,不受约束的补体激活可能会触发自组织损伤,从而导致病理状况。在这三种补体激活途径中,替代途径(AP)特别涉及许多疾病和损伤状态。因此,AP组分代表了治疗干预的有吸引力的靶标。 I科(Ixodidae)常见的硬tick是从其哺乳动物宿主的血液中获取营养。在其血粉中,tick暴露于宿主免疫效应子,包括补体系统。在防御中,壁虱产生的唾液蛋白可以抑制宿主的免疫功能。肩x骨的Salp20唾液蛋白通过结合备解素和解离活性C3转化酶C3bBbP来抑制宿主AP途径。在这些研究中,我们研究了Salp20在各种补体介导的病理学中的活性。我们的结果表明Salp20可以抑制小鼠AP依赖的发病机理。它的功效可能部分归因于它与内源性AP调节剂H因子的协同作用。虽然Salp20本身被认为具有高度免疫原性,因此不适用于治疗用途,但它的出现说明了非免疫原性的潜在发展Salp20模拟物复制其抗备解素活性。

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