白细胞介素-4的拮抗突变蛋白。

Behring Institute Mitteilungen Pub Date : 1995-06-01
A Duschl, T Müller, W Sebald
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引用次数: 0

摘要

白细胞介素-4是免疫系统的主要调节因子,例如引导t细胞中TH2表型的诱导,b细胞的激活和与过敏反应相关的IgE型抗体的合成。位点定向诱变揭示了IL-4受体相互作用的两个重要位点:位点I介导与IL-4受体α亚基的结合,位点II通过受体复合物参与信号转导。II位点的特异性突变产生了一系列高亲和力结合受体的配体,但对野生型IL-4几乎没有或没有激动活性和抑制作用。密切相关的细胞因子IL-13,也是过敏过程的中介,也被拮抗。因此,人类IL-4的拮抗II位点突变体是有效的抑制剂,具有治疗IL-4相关疾病的潜力,如I型超敏反应和哮喘。
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Antagonistic mutant proteins of interleukin-4.

Interleukin-4 is a major regulator of the immune system, directing e.g. induction of a TH2 phenotype in T-cells, activation of B-cells and synthesis of IgE type antibodies, which are associated with allergic responses. Site-directed mutagenesis has revealed two sites important for receptor interaction on IL-4: site I mediates binding to the IL-4 receptor alpha subunit, and site II is involved in signal transduction through the receptor complex. Specific mutations in site II produced a series of ligands which bound to the receptor with high affinity, but had little or no agonistic activity and inhibited effects of wild type IL-4. The closely related cytokine IL-13, also a mediator of allergic processes, is antagonized as well. Antagonistic site II mutants of human IL-4 are therefore effective inhibitors with therapeutic potential for IL-4 associated diseases like type I hypersensitivity and asthma.

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