首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Systemic administration of an Fcgamma-Fc(epsilon)-fusion protein in house dust mite sensitive nonhuman primates.
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Systemic administration of an Fcgamma-Fc(epsilon)-fusion protein in house dust mite sensitive nonhuman primates.

机译:在室内尘螨敏感的非人类灵长类动物中全身施用Fcgamma-Fc(ε)融合蛋白。

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摘要

Crosslinking Fc(epsilon)RI and FcgammaRIIB receptors inhibits mast cell and basophil activation, decreasing mediator release. In this study, a fusion protein incorporating human Fcgamma and Fc(epsilon) domains, hGE2, was shown to inhibit degranulation of human mast cells and basophils, and to exhibit efficacy in a nonhuman primate model of allergic asthma. hGE2 increased the provocative concentration of dust mite aeroallergen that induced an early phase asthmatic response. The treatment effect lasted up to 4 weeks and was associated with reduction in the number of circulating basophils and decreased expression of Fc(epsilon)RI on repopulating basophils. Repeat hGE2 dosing induced production of serum antibodies against human Fcgamma and Fc(epsilon) domains and acute anaphylaxis-like reactions. Immune serum induced histamine release from human IgE or hGE2-treated cord blood-derived mast cells and basophils in vitro. These results indicate that repeat administration with hGE2 induced an antibody response to the human molecule that resulted in activation rather than inhibition of allergic responses.
机译:交联的Fc(ε)RI和FcgRIRIIB受体抑制肥大细胞和嗜碱性粒细胞活化,从而减少介质释放。在这项研究中,融合人Fcγ和Fc(ε)域hGE2的融合蛋白显示抑制人肥大细胞和嗜碱性粒细胞脱粒,并在过敏性哮喘的非人灵长类动物模型中显示出功效。 hGE2增加了引起早期哮喘反应的尘螨气敏原的刺激性浓度。该治疗效果持续长达4周,与循环嗜碱细胞数量的减少和Fc(ε)RI在重生嗜碱细胞上的表达降低有关。重复hGE2剂量诱导针对人Fcγ和Fc(ε)域的血清抗体的产生以及急性过敏样反应。免疫血清诱导组胺从人IgE或hGE2处理的脐血来源的肥大细胞和嗜碱细胞中释放。这些结果表明,用hGE2重复施用诱导了对人分子的抗体应答,导致活化而不是抑制了过敏反应。

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