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IL-8 single-chain homodimers and heterodimers: interactions with chemokine receptors CXCR1, CXCR2, and DARC.

机译:IL-8单链同二聚体和异二聚体:与趋化因子受体CXCR1,CXCR2和DARC的相互作用。

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摘要

Covalent single-chain dimers of the chemokine interleukin-8 (IL-8) have been designed to mimic the dimeric form of IL-8 in solution and facilitate the production of heterodimer variants of IL-8. Physical studies indicated that use of a simple peptide linker to join two subunits, while allowing receptor binding and activation, led to self-association of the tethered dimers. However, addition of a single disulfide crosslink between the tethered subunits prevented this multimer from forming, yielding a species of dimer molecular weight. Crosslinked single-chain dimers bind to both IL-8 neutrophil receptors CXCR1 and CXCR2 as well as to DARC, as does a double disulfide-linked dimer with no peptide linker. In addition, neutrophil response to these dimers as measured by chemotaxis or beta-glucuronidase release is similar to that elicited by wild-type IL-8, providing evidence that the dissociation of the dimeric species is not required for these biologically relevant activities. Finally, through construction of single-chain heterodimer mutants, we show that only the first subunit's ELR motif is the single-chain variants.
机译:已设计趋化因子白介素8(IL-8)的共价单链二聚体,以模拟溶液中IL-8的二聚体形式,并促进IL-8异二聚体变体的生产。物理研究表明,使用简单的肽接头连接两个亚基,同时允许受体结合和激活,可导致束缚二聚体的自缔合。然而,在束缚的亚基之间添加单个二硫键交联阻止了该多聚体的形成,从而产生了一种二聚体分子量。交联的单链二聚体与IL-8中性粒细胞受体CXCR1和CXCR2以及DARC都结合,双二硫键连接的无肽接头的二聚体也是如此。另外,通过趋化性或β-葡糖醛酸糖苷酶释放测量的对这些二聚体的嗜中性粒细胞应答类似于野生型IL-8引起的嗜中性粒细胞应答,提供了证据表明这些生物学相关活性不需要二聚体物种的解离。最后,通过构建单链异二聚体突变体,我们表明只有第一个亚基的ELR基序是单链变体。

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