Small RNA sequencing analysis reveals regulation of microRNA expression in Madin-Darby canine kidney epithelial cells infected with Canid alphaherpesvirus 1.

IF 1.9 4区 医学 Q3 GENETICS & HEREDITY
Virus Genes Pub Date : 2024-10-01 Epub Date: 2024-07-17 DOI:10.1007/s11262-024-02091-6
Maha Ben Hamouda, Angela Pearson
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引用次数: 0

Abstract

Canid alphaherpesvirus 1 (CHV-1) infection can cause spontaneous abortions in pregnant dams, and in young puppies, fatal systemic infections are common. MicroRNAs (miRNAs) affect viral infection by binding to messenger RNAs, and inhibiting expression of host and/or viral genes. We conducted deep sequencing of small RNAs in CHV-1-infected and mock-infected Madin-Darby Canine Kidney (MDCK) epithelial cells, and detected sequences corresponding to 282 cellular miRNAs. Of these, 18 were significantly upregulated at 12 h post-infection, most of which were encoded on the X chromosome. We next quantified the mature forms of several of the miRNAs using stem loop RT-qPCR. Our results revealed a discordance between the levels of small RNAs corresponding to canine miRNAs, and levels of the corresponding mature miRNAs, which suggests a block in miRNA biogenesis in infected cells. Nevertheless, we identified several mature miRNAs that exhibited a statistically significant increase upon infection. These included cfa-miR-8908b, a miRNA of unknown function, and cfa-miR-146a, homologs of which target innate immune pathways and are known to play a role in other viral infections. Interestingly, ontology analysis predicted that cfa-miR-8908b targets factors involved in the ubiquitin-like protein conjugation pathway and peroxisome biogenesis among other cellular functions. This is the first study to evaluate changes in miRNA levels upon CHV-1 infection. Based on our findings, we developed a model whereby CHV-1 infection results in changes in levels of a limited number of cellular miRNAs that target elements of the host immune response, which may provide clues regarding novel therapeutic targets.

Abstract Image

小核糖核酸测序分析揭示了感染犬α疱疹病毒 1 的马丹达比犬肾上皮细胞中微小核糖核酸表达的调控。
犬甲型疱疹病毒 1(CHV-1)感染可导致怀孕母犬自然流产,幼犬感染致命的全身性感染也很常见。微RNA(miRNA)通过与信使RNA结合,抑制宿主和/或病毒基因的表达,从而影响病毒感染。我们对感染 CHV-1 和模拟感染 Madin-Darby 犬肾 (MDCK) 上皮细胞中的小 RNA 进行了深度测序,检测到 282 个细胞 miRNA 的相应序列。其中有 18 种 miRNA 在感染后 12 小时明显上调,它们大多在 X 染色体上编码。接下来,我们利用干环 RT-qPCR 对几种 miRNA 的成熟形式进行了量化。我们的结果显示,与犬 miRNA 相对应的小 RNA 水平与相应的成熟 miRNA 水平不一致,这表明感染细胞中的 miRNA 生物发生受阻。尽管如此,我们还是发现了几种成熟的 miRNA 在感染后出现了统计学意义上的显著增加。其中包括功能未知的 miRNA cfa-miR-8908b 和 cfa-miR-146a,它们的同源物靶向先天性免疫通路,已知在其他病毒感染中发挥作用。有趣的是,本体分析预测,cfa-miR-8908b 以参与泛素样蛋白共轭途径和过氧物酶体生物生成等细胞功能的因子为靶标。这是第一项评估感染 CHV-1 后 miRNA 水平变化的研究。根据我们的研究结果,我们建立了一个模型,在这个模型中,CHV-1 感染会导致以宿主免疫反应要素为靶点的数量有限的细胞 miRNA 水平发生变化,这可能会为新的治疗靶点提供线索。
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来源期刊
Virus Genes
Virus Genes 医学-病毒学
CiteScore
3.30
自引率
0.00%
发文量
76
审稿时长
3 months
期刊介绍: Viruses are convenient models for the elucidation of life processes. The study of viruses is again on the cutting edge of biological sciences: systems biology, genomics, proteomics, metagenomics, using the newest most powerful tools. Huge amounts of new details on virus interactions with the cell, other pathogens and the hosts – animal (including human), insect, fungal, plant, bacterial, and archaeal - and their role in infection and disease are forthcoming in perplexing details requiring analysis and comments. Virus Genes is dedicated to the publication of studies on the structure and function of viruses and their genes, the molecular and systems interactions with the host and all applications derived thereof, providing a forum for the analysis of data and discussion of its implications, and the development of new hypotheses.
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