首页> 外文期刊>Immunity >Structure of the human IgE-Fc C epsilon 3-C epsilon 4 reveals conformational flexibility in the antibody effector domains.
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Structure of the human IgE-Fc C epsilon 3-C epsilon 4 reveals conformational flexibility in the antibody effector domains.

机译:人IgE-Fc C epsilon 3-C epsilon 4的结构揭示了抗体效应子域中的构象柔性。

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摘要

IgE antibodies mediate antiparasitic immune responses and the inflammatory reactions of allergy and asthma. We have solved the crystal structure of the human IgE-Fc Cepsilon3-Cepsilon4 domains to 2.3 A resolution. The structure reveals a large rearrangement of the N-terminal Cepsilon3 domains when compared to related IgG-Fc structures and to the IgE-Fc bound to its high-affinity receptor, FcepsilonRI. The IgE-Fc adopts a more compact, closed configuration that places the two Cepsilon3 domains in close proximity, decreases the size of the interdomain cavity, and obscures part of the FcepsilonRI binding site. IgE-Fc conformational flexibility may be required for interactions with two distinct IgE receptors, and the structure suggests strategies for the design of therapeutic compounds for the treatment of IgE-mediated diseases.
机译:IgE抗体介导抗寄生虫免疫反应以及过敏和哮喘的炎症反应。我们已经解决了人类IgE-Fc Cepsilon3-Cepsilon4域的晶体结构,分辨率达到2.3A。与相关的IgG-Fc结构以及与其高亲和力受体FcepsilonRI结合的IgE-Fc相比,该结构揭示了N-末端Cepsilon3结构域的重排。 IgE-Fc采用更紧凑的封闭构型,将两个Cepsilon3结构域紧密相邻,减小了结构域腔的大小,并遮盖了FcepsilonRI结合位点的一部分。与两个不同的IgE受体相互作用可能需要IgE-Fc构象柔韧性,并且该结构提出了设计用于治疗IgE介导的疾病的治疗性化合物的策略。

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