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首页> 外文期刊>Immunology Letters >Inhibition of human cord blood-derived mast cell responses by anti-Fc epsilon RI mAb 15/1 versus anti-IgE Omalizumab.
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Inhibition of human cord blood-derived mast cell responses by anti-Fc epsilon RI mAb 15/1 versus anti-IgE Omalizumab.

机译:与抗IgE奥马珠单抗相比,抗FcεRI单克隆抗体15/1对人脐带血肥大细胞反应的抑制作用。

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摘要

Aggregation of the alpha-chain of the high affinity IgE receptor (Fc epsilon RI alpha) on mast cells or basophils after cross-linking of receptor-bound IgE by its antigen or an anti-IgE antibody results in cell activation and release of inflammatory mediators. Omalizumab (Xolair), Novartis Pharmaceuticals; Genentech Inc.) is a recombinant humanized anti-IgE mAb developed for the treatment of severe allergic asthma. It complexes with free serum IgE, which prevents its binding to Fc epsilon RI and thereby interrupts the allergic cascade. Administration of an inhibitory anti-Fc epsilon RI alpha mAb may represent an alternative strategy to neutralize IgE-mediated receptor activation. In the present report, for the first time, we have performed direct side of side comparison between the inhibitory anti-Fc epsilon RI alpha mAb designated 15/1 and Omalizumab for their effects on human cord blood-derived mast cells. We provide the first evidence that both 15/1 mAb and Omalizumab efficiently inhibit Fc epsilon RI-mediated human mast cell responses in vitro (degranulation, activation, release of IL-8 and IL-13, phosphorylation of Akt) and that mAb 15/1 is a non-anaphylactogenic antibody, which compared to Omalizumab, displays markedly higher inhibitory potency in the presence of high IgE levels.
机译:受体结合的IgE通过其抗原或抗IgE抗体交联后,肥大细胞或嗜碱性粒细胞上高亲和力IgE受体(Fc epsilon RI alpha)的α链聚集导致细胞活化和炎性介质的释放。诺华制药的Omalizumab(Xolair); Genentech Inc.)是一种用于治疗严重过敏性哮喘的重组人源化抗IgE mAb。它与游离血清IgE形成复合物,从而阻止其与FcεRI结合,从而中断了过敏级联反应。抑制性抗FcεRIαmAb的给药可能代表了中和IgE介导的受体激活的替代策略。在本报告中,我们首次对命名为15/1的抑制性抗FcεRIαmAb和Omalizumab对人脐血来源的肥大细胞的作用进行了直接的侧面比较。我们提供了第一个证据,即15/1 mAb和Omalizumab均可在体外有效抑制FcεRI介导的人类肥大细胞反应(脱粒,活化,IL-8和IL-13的释放,Akt的磷酸化),以及mAb 15 / 1是非过敏原性抗体,与Omalizumab相比,在高IgE水平下显示出明显更高的抑制效力。

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