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来自不同属的蜱虫编码趋化因子抑制蛋白evasin。

Ticks from diverse genera encode chemokine-inhibitory evasin proteins.

作者信息

Hayward Jenni, Sanchez Julie, Perry Andrew, Huang Cheng, Rodriguez Valle Manuel, Canals Meritxell, Payne Richard J, Stone Martin J

机构信息

From the Infection and Immunity Program, Monash Biomedicine Discovery Institute, and Department of Biochemistry and Molecular Biology and.

the Monash Bioinformatics Platform, Monash University, Clayton, Victoria 3800, Australia.

出版信息

J Biol Chem. 2017 Sep 22;292(38):15670-15680. doi: 10.1074/jbc.M117.807255. Epub 2017 Aug 4.

Abstract

To prolong residence on their hosts, ticks secrete many salivary factors that target host defense molecules. In particular, the tick has been shown to produce three salivary glycoproteins named "evasins," which bind to host chemokines, thereby inhibiting the recruitment of leukocytes to the location of the tick bite. Using sequence similarity searches, we have identified 257 new putative evasin sequences encoded by the genomes or salivary or visceral transcriptomes of numerous hard ticks, spanning the genera , , and of the Ixodidae family. Nine representative sequences were successfully expressed in , and eight of the nine candidates exhibited high-affinity binding to human chemokines. Sequence alignments enabled classification of the evasins into two subfamilies: C evasins share a conserved set of eight Cys residues (four disulfide bonds), whereas C evasins have only three of these disulfide bonds. Most of the identified sequences contain predicted secretion leader sequences, -linked glycosylation sites, and a putative site of tyrosine sulfation. We conclude that chemokine-binding evasin proteins are widely expressed among tick species of the Ixodidae family, are likely to play important roles in subverting host defenses, and constitute a valuable pool of anti-inflammatory proteins for potential future therapeutic applications.

摘要

为了延长在宿主身上的停留时间,蜱虫会分泌多种针对宿主防御分子的唾液因子。特别是,已证明蜱虫会产生三种名为“逃避素”的唾液糖蛋白,它们与宿主趋化因子结合,从而抑制白细胞向蜱虫叮咬部位募集。通过序列相似性搜索,我们在多种硬蜱的基因组、唾液或内脏转录组中鉴定出257个新的假定逃避素序列,这些硬蜱涵盖硬蜱科的 属、 属和 属。九个代表性序列在 中成功表达,九个候选序列中的八个对人类趋化因子表现出高亲和力结合。序列比对使逃避素能够分为两个亚家族:C逃避素共有一组保守的八个半胱氨酸残基(四个二硫键),而C逃避素只有其中三个二硫键。大多数鉴定出的序列包含预测的分泌前导序列、 连接的糖基化位点和一个假定的酪氨酸硫酸化位点。我们得出结论,趋化因子结合逃避素蛋白在硬蜱科的蜱虫物种中广泛表达,可能在颠覆宿主防御中发挥重要作用,并构成了一个有价值的抗炎蛋白库,可用于未来潜在的治疗应用。

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