首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Enhanced Effector Functions Due to Antibody Defucosylation Depend on the Effector Cell Fc gamma Receptor Profile
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Enhanced Effector Functions Due to Antibody Defucosylation Depend on the Effector Cell Fc gamma Receptor Profile

机译:增强型效应器函数由于抗体脓性溶胶化取决于效应细胞Fcγcacecor曲线

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摘要

Abs of the IgG isotype are glycosylated in their Fc domain at a conserved asparagine at position 297. Removal of the core fucose of this glycan greatly increases the affinity for Fc gamma RIII, resulting in enhanced Fc gamma RIII-mediated effector functions. Normal plasma IgG contains similar to 94% fucosylated Abs, but alloantibodies against, for example, Rhesus D (RhD) and platelet Ags frequently have reduced fucosylation that enhances their pathogenicity. The increased FcgRIII-mediated effector functions have been put to use in various afucosylated therapeutic Abs in anticancer treatment. To test the functional consequences of Ab fucosylation, we produced V-gene-matched recombinant anti-RhD IgG Abs of the four different subclasses (IgG1-4) with and without core fucose (i.e., 20% fucose remaining). Binding to all human Fc gamma R types and their functional isoforms was assessed with surface plasmon resonance. All hypofucosylated anti-RhD IgGs of all IgG subclasses indeed showed enhanced binding affinity for isolated FcgRIII isoforms, without affecting binding affinity to other Fc gamma Rs. In contrast, when testing hypofucosylated anti-RhD Abs with Fc gamma RIIIaexpressing NK cells, a 12-and 7-fold increased erythrocyte lysis was observed with the IgG1 and IgG3, respectively, but no increase with IgG2 and IgG4 anti-RhD Abs. Notably, none of the hypofucosylated IgGs enhanced effector function of macrophages, which, in contrast to NK cells, express a complex set of FcgRs, including Fc gamma RIIIa. Our data suggest that the beneficial effects of afucosylated biologicals for clinical use can be anticipated when there is a substantial involvement of Fc gamma RIIIa-expressing cells, such as NK cells.
机译:将IgG同种型的ABS在其Fc结构域中在777的保守天才中糖基化。除去该甘油的核心岩糖大大增加了对FcγRIII的亲和力,导致增强的FcγRIII介导的效应器功能。正常等离子体IgG含有类似于94%的岩藻糖基化的ABS,但是,例如恒河猴和血小板AGS的含量较低,岩藻糖基化量降低,其增强其致病性。增加了FcGRIII介导的效应功能,以抗癌治疗中的各种逐渐消耗的治疗腹肌。为了测试AB岩藻糖基化的功能后果,我们生产的V-Gene匹配的重组抗RHD IgG ABS的四种不同亚类(IgG1-4)的具有,无核心岩糖(即20%岩藻糖)。用表面等离子体共振评估与所有人FCγγ型和其功能同种型的结合。所有IgG亚亚类的所有低琥珀酰化的抗RHD IgG确实显示出对分离的FcGRII同种型的增强的结合亲和力,而不影响其它FcγRS的结合亲和力。相反,当用FcγRIIIA表达的NK细胞测试低酸化囊化的抗rhD ABS时,分别用IgG1和IgG3观察到12-倍和7倍的红细胞裂解,但与IgG2和IgG4抗RHD ABS增加。值得注意的是,巨毛囊化的IgGs没有一种增强巨噬细胞的效应函数,与NK细胞相反,表达了一种复杂的FCGR,包括FcγRIIIA。我们的数据表明,当存在显着涉及FcγRIIIa的细胞(例如NK细胞)时,可以预期临床用途对临床用途的有益效果。

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