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对新发现的蜱唾液特异性微小RNA进行的计算机靶标网络分析揭示了它们在干扰脊椎动物宿主生理过程中的重要组合效应。

In silico target network analysis of de novo-discovered, tick saliva-specific microRNAs reveals important combinatorial effects in their interference with vertebrate host physiology.

作者信息

Hackenberg Michael, Langenberger David, Schwarz Alexandra, Erhart Jan, Kotsyfakis Michail

机构信息

Computational Genomics and Bioinformatics Group, Genetics Department, University of Granada, 18071 Granada, Spain.

Laboratorio de Bioinformática, Centro de Investigación Biomédica, PTS, 18100 Granada, Spain.

出版信息

RNA. 2017 Aug;23(8):1259-1269. doi: 10.1261/rna.061168.117. Epub 2017 May 4.

Abstract

The hard tick is an important disease vector whose salivary secretions mediate blood-feeding success on vertebrate hosts, including humans. Here we describe the expression profiles and downstream analysis of de novo-discovered microRNAs (miRNAs) expressed in salivary glands and saliva. Eleven tick-derived libraries were sequenced to produce 67,375,557 Illumina reads. De novo prediction yielded 67 bona fide miRNAs out of which 35 are currently not present in miRBase. We report for the first time the presence of microRNAs in tick saliva, obtaining furthermore molecular indicators that those might be of exosomal origin. Ten out of these microRNAs are at least 100 times more represented in saliva. For the four most expressed microRNAs from this subset, we analyzed their combinatorial effects upon their host transcriptome using a novel in silico target network approach. We show that only the inclusion of combinatorial effects reveals the functions in important pathways related to inflammation and pain sensing. A control set of highly abundant microRNAs in both saliva and salivary glands indicates no significant pathways and a far lower number of shared target genes. Therefore, the analysis of miRNAs from pure tick saliva strongly supports the hypothesis that tick saliva miRNAs can modulate vertebrate host homeostasis and represents the first direct evidence of tick miRNA-mediated regulation of vertebrate host gene expression at the tick-host interface. As such, the herein described miRNAs may support future drug discovery and development projects that will also experimentally question their predicted molecular targets in the vertebrate host.

摘要

硬蜱是一种重要的疾病传播媒介,其唾液分泌物有助于在包括人类在内的脊椎动物宿主身上成功取食。在此,我们描述了在唾液腺和唾液中从头发现的微小RNA(miRNA)的表达谱及下游分析。对11个蜱源文库进行测序,产生了67375557条Illumina读数。从头预测产生了67个真正的miRNA,其中35个目前在miRBase中不存在。我们首次报道了蜱唾液中存在微小RNA,此外还获得了表明这些微小RNA可能来源于外泌体的分子指标。其中有10种微小RNA在唾液中的表达量至少高出100倍。对于该亚组中表达量最高的4种微小RNA,我们使用一种新的计算机模拟靶标网络方法分析了它们对宿主转录组的组合效应。我们发现,只有纳入组合效应才能揭示与炎症和疼痛感知相关的重要途径中的功能。唾液和唾液腺中一组高度丰富的对照微小RNA显示没有显著的途径,且共享靶基因的数量要少得多。因此,对纯蜱唾液中miRNA的分析有力地支持了蜱唾液miRNA可调节脊椎动物宿主内环境稳定的假说,并代表了蜱miRNA在蜱 - 宿主界面介导脊椎动物宿主基因表达调控的首个直接证据。因此,本文所述的miRNA可能会支持未来的药物发现和开发项目,这些项目也将通过实验对它们在脊椎动物宿主中的预测分子靶标提出质疑。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c8dc/5513070/38bc8ac4f691/1259f01.jpg

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