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酵母表面展示技术鉴定了来自蜱虫的一系列逃避蛋白,它们具有新型的多价 CC 趋化因子结合活性。

Yeast surface display identifies a family of evasins from ticks with novel polyvalent CC chemokine-binding activities.

机构信息

RDM Division of Cardiovascular Medicine and Wellcome Trust Centre for Human Genetics, University of Oxford, Roosevelt Drive, Oxford, OX3 7BN, United Kingdom.

Dept of Chemistry, University of Oxford, Mansfield Road, Oxford, OX1 3TA, United Kingdom.

出版信息

Sci Rep. 2017 Jun 27;7(1):4267. doi: 10.1038/s41598-017-04378-1.

Abstract

Chemokines function via G-protein coupled receptors in a robust network to recruit immune cells to sites of inflammation. Due to the complexity of this network, targeting single chemokines or receptors has not been successful in inflammatory disease. Dog tick saliva contains polyvalent CC-chemokine binding peptides termed evasins 1 and 4, that efficiently disrupt the chemokine network in models of inflammatory disease. Here we develop yeast surface display as a tool for functionally identifying evasins, and use it to identify 10 novel polyvalent CC-chemokine binding evasin-like peptides from salivary transcriptomes of eight tick species in Rhipicephalus and Amblyomma genera. These evasins have unique binding profiles compared to evasins 1 and 4, targeting CCL2 and CCL13 in addition to other CC-chemokines. Evasin binding leads to neutralisation of chemokine function including that of complex chemokine mixtures, suggesting therapeutic efficacy in inflammatory disease. We propose that yeast surface display is a powerful approach to mine potential therapeutics from inter-species protein interactions that have arisen during evolution of parasitism in ticks.

摘要

趋化因子通过 G 蛋白偶联受体在一个强大的网络中发挥作用,将免疫细胞募集到炎症部位。由于这个网络的复杂性,针对单一趋化因子或受体在炎症性疾病中并没有成功。狗蜱唾液中含有多价 C 型趋化因子结合肽,称为逃逸素 1 和 4,可有效破坏炎症性疾病模型中的趋化因子网络。在这里,我们开发了酵母表面展示作为一种功能鉴定逃逸素的工具,并利用它从 Rhipicephalus 和 Amblyomma 属的 8 种蜱的唾液转录组中鉴定出 10 种新型多价 C 型趋化因子结合逃逸素样肽。与逃逸素 1 和 4 相比,这些逃逸素具有独特的结合谱,除了其他 C 型趋化因子外,还靶向 CCL2 和 CCL13。逃逸素结合导致趋化因子功能被中和,包括复杂趋化因子混合物的功能,这表明在炎症性疾病中具有治疗效果。我们提出,酵母表面展示是一种从蜱寄生进化过程中产生的种间蛋白质相互作用中挖掘潜在治疗药物的有力方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0161/5487423/44d96f814169/41598_2017_4378_Fig1_HTML.jpg

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