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Microarray-based transcriptional profiling of Eimeria bovis-infected bovine endothelial host cells

机译:基于微阵列的牛艾美球虫感染的牛内皮宿主细胞的转录概况分析

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摘要

Within its life cycle Eimeria bovis undergoes a long lasting intracellular development into large macromeronts in endothelial cells. Since little is known about the molecular basis of E. bovis-triggered host cell regulation we applied a microarray-based approach to define transcript variation in bovine endothelial cells early after sporozoite invasion (4 h post inoculation (p.i.)), during trophozoite establishment (4 days p.i.), during early parasite proliferation (8 days p.i.) and towards macromeront maturation (14 days p.i.). E. bovis infection led to significant changes in the abundance of many host cell gene transcripts. As infection progressed, the number of regulated genes increased such that 12, 45, 175 and 1184 sequences were modulated at 4 h, 4, 8 and 14 days p.i., respectively. These genes significantly interfered with several host cell functions, networks and canonical pathways, especially those involved in cellular development, cell cycle, cell death, immune response and metabolism. The correlation between stage of infection and the number of regulated genes involved in different aspects of metabolism suggest parasite-derived exploitation of host cell nutrients. The modulation of genes involved in cell cycle arrest and host cell apoptosis corresponds to morphological in vitro findings and underline the importance of these aspects for parasite survival. Nevertheless, the increasing numbers of modulated transcripts associated with immune responses also demonstrate the defensive capacity of the endothelial host cell. Overall, this work reveals a panel of novel candidate genes involved in E. bovis-triggered host cell modulation, providing a valuable tool for future work on this topic.
机译:在其生命周期中,牛艾美尔球虫在内皮细胞中经历了长期持续的细胞内发育,变成了大的巨单体。由于对牛大肠杆菌触发的宿主细胞调节的分子基础知之甚少,我们在滋养体建立期间(在接种子后(pi)接种后4小时)应用了基于微阵列的方法来定义牛内皮细胞转录本的变化( pi 4天),早期寄生虫增殖(pi 8天)和大单体成熟(pi 14天)。牛大肠杆菌感染导致许多宿主细胞基因转录本的丰度发生显着变化。随着感染的进行,调节基因的数量增加,使得分别在p.i. 4 h,4、8和14天分别调节12、45、175和1184个序列。这些基因显着干扰了几种宿主细胞的功能,网络和经典途径,特别是那些参与细胞发育,细胞周期,细胞死亡,免疫应答和代谢的细胞。感染的阶段与代谢的不同方面所涉及的调控基因数量之间的相关性表明,寄生虫可以利用宿主细胞中的营养物质。参与细胞周期停滞和宿主细胞凋亡的基因调节与体外形态学发现相对应,并强调了这些方面对于寄生虫存活的重要性。然而,与免疫应答相关的调节转录本的数量增加也证明了内皮宿主细胞的防御能力。总的来说,这项工作揭示了一组涉及牛大肠杆菌触发的宿主细胞调控的新候选基因,为该主题的未来工作提供了有价值的工具。

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