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Nasonia vitripennis venom causes targeted gene expression changes in its fly host

机译:Nasonia vitripennis毒液在其蝇宿主中引起定向基因表达变化

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摘要

Parasitoid wasps are diverse and ecologically important insects that use venom to modify their host’s metabolism for the benefit of the parasitoid’s offspring. Thus, the effects of venom can be considered an ‘extended phenotype’ of the wasp. The model parasitoid wasp Nasonia vitripennis has approximately 100 venom proteins, 23 of which do not have sequence similarity to known proteins. Envenomation by N. vitripennis has previously been shown to induce developmental arrest, selective apoptosis and alterations in lipid metabolism in flesh fly hosts. However, the full effects of Nasonia venom are still largely unknown. In this study, we used high throughput RNA sequencing (RNA-Seq) to characterize global changes in Sarcophaga bullata (Diptera) gene expression in response to envenomation by N. vitripennis. Surprisingly, we show that Nasonia venom targets a small subset of S. bullata loci, with ~2% genes being differentially expressed in response to envenomation. Strong upregulation of enhancer of split complex genes provides a potential molecular mechanism that could explain the observed neural cell death and developmental arrest in envenomated hosts. Significant increases in antimicrobial peptides and their corresponding regulatory genes provide evidence that venom could be selectively activating certain immune responses of the hosts. Further, we found differential expression of genes in several metabolic pathways, including glycolysis and gluconeogenesis that may be responsible for the decrease in pyruvate levels found in envenomated hosts. The targeting of Nasonia venom effects to a specific and limited set of genes provides insight into the interaction between the ectoparasitoid wasp and its host.
机译:寄生性黄蜂是多种多样且具有重要生态意义的昆虫,它们利用毒液改变宿主的新陈代谢,从而使寄生性黄蜂的后代受益。因此,毒液的作用可以被认为是黄蜂的“扩展表型”。拟寄生物黄蜂模型Nasonia vitripennis具有大约100种毒液蛋白,其中23种与已知蛋白没有序列相似性。以前已显示出通过玻璃纸猪笼草的毒化可以诱导果蝇宿主发育停滞,选择性凋亡和脂质代谢的改变。然而,Nasonia毒液的全部作用仍然很大程度上未知。在这项研究中,我们使用高通量RNA测序(RNA-Seq)来表征响应沙门氏菌(N. vitripennis)的毒化而在大石棺(Diptera)基因表达中的总体变化。出乎意料的是,我们显示纳索尼亚毒液以一小部分的大牛链球菌基因座为目标,其中约2%的基因响应于毒化反应而差异表达。分裂的复杂基因增强子的强烈上调提供了潜在的分子机制,可以解释观察到的宿主细胞中神经细胞的死亡和发育停滞。抗菌肽及其相应调控基因的显着增加提供了证据,表明毒液可以选择性激活宿主的某些免疫反应。此外,我们发现了基因在几种代谢途径中的差异表达,包括糖酵解和糖异生,这可能是导致宿主体内丙酮酸水平降低的原因。将Nasonia毒液作用针对特定和有限的一组基因,可以深入了解类外寄生虫黄蜂与其宿主之间的相互作用。

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