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Complement Component C3 Binds to the A3 Domain of von Willebrand Factor

机译:补体成分C3与von Willebrand因子的A3域结合

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摘要

von Willebrand factor (VWF) is a multimeric protein composed of monomeric subunits (∼280 kD) linked by disulfide bonds. During hemostasis and thrombosis, ultralarge (UL) VWF (ULVWF) multimers initiate platelet adhesion. In vitro, human C3 binds to ULVWF multimeric strings secreted by and anchored to human endothelial cell to promote the assembly and activation of C3 convertase (C3bBb) and C5 convertase (C3bBbC3b) of the alternative complement pathway (AP). The purified and soluble C3 avidly binds to recombinant human VWF A1A2A3, as well as the recombinant isolated human VWF A3 domain. Notably, the binding of soluble human ULVWF multimers to purified human C3 was blocked by addition of a monovalent Fab fragment antibody to the VWF A3 domain. We conclude that the A3 domain in VWF/ULVWF contains a docking site for C3. In contrast, purified human C4, an essential component of the classical and lectin complement pathways, binds to soluble, isolated A1, but not to ULVWF strings secreted by and anchored to endothelial cells. Our findings should facilitate the design of new therapeutic agents to suppress the initiation of the AP on ULVWF multimeric strings during thrombotic and inflammatory disorders.
机译:von Willebrand因子(VWF)是一种多聚体蛋白,由通过二硫键连接的单体亚基(〜280 kD)组成。在止血和血栓形成过程中,超大型(UL)VWF(ULVWF)多聚体会引发血小板粘附。在体外,人C3结合由人内皮细胞分泌并锚定在其上的ULVWF多聚体链,以促进旁路补体途径(AP)的C3转化酶(C3bBb)和C5转化酶(C3bBbC3b)的组装和激活。纯化且可溶的C3与重组人VWF A1A2A3以及重组分离的人VWF A3结构域紧密结合。值得注意的是,可溶的人ULVWF多聚体与纯化的人C3的结合通过向VWF A3结构域添加单价Fab片段抗体而被阻断。我们得出结论,VWF / ULVWF中的A3域包含C3的停靠站点。相反,纯化的人C4是经典和凝集素补体途径的重要组成部分,与可溶的,分离的A1结合,但不与内皮细胞分泌并锚定的ULVWF弦结合。我们的发现应有助于设计新的治疗剂,以抑制血栓性和炎性疾病期间ULVWF多聚体弦上AP的启动。

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