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具有生物活性的白细胞介素-5单体的构建。

Creation of a biologically active interleukin-5 monomer.

作者信息

Dickason R R, Huston D P

机构信息

Baylor College of Medicine, Department of Medicine, Houston, Texas 77030, USA.

出版信息

Nature. 1996 Feb 15;379(6566):652-5. doi: 10.1038/379652a0.

Abstract

Interleukin-5 (IL-5) specifically induces the differentiation of eosinophils, which are important in host defence and the pathogenesis of allergies and asthma. Structurally, IL-5 is a unique member of the short-chain helical-bundle subfamily of cytokines whose canonical motif contains four helices (A-D) arranged in an up-up-down-down topology. In contrast to other subfamily members, which fold unimolecularly into a single helical bundle, IL-5 forms a pair of helical bundles by the interdigitation of two identical monomers that contribute a D helix to the other's A-C helices. We predicted that the lack of bioactivity by an IL-5 monomer was due to a short loop between helices C and D which physically prevents unimolecular folding of helix D into a functionally obligate structural motif. Here we report that, by lengthening this loop, we have engineered an insertional mutant of IL-5 that was expressed as a monomer with biological activity similar to that of native IL-5. These studies demonstrate that all of the structural features necessary for IL-5 to function are contained within a single helical bundle.

摘要

白细胞介素-5(IL-5)特异性诱导嗜酸性粒细胞的分化,嗜酸性粒细胞在宿主防御以及过敏和哮喘的发病机制中起重要作用。从结构上看,IL-5是细胞因子短链螺旋束亚家族的独特成员,其典型基序包含以上下上下拓扑结构排列的四个螺旋(A-D)。与其他单分子折叠成单个螺旋束的亚家族成员不同,IL-5通过两个相同单体的相互交错形成一对螺旋束,每个单体为另一个单体的A-C螺旋贡献一个D螺旋。我们推测IL-5单体缺乏生物活性是由于螺旋C和D之间的短环,该短环在物理上阻止了螺旋D单分子折叠成功能上必需的结构基序。在此我们报告,通过延长这个环,我们构建了一个IL-5插入突变体,其作为具有与天然IL-5相似生物活性的单体表达。这些研究表明,IL-5发挥功能所需的所有结构特征都包含在单个螺旋束中。

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