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鸡体内干扰素调节基因的组织和时间特异性表达模式

Tissue and time specific expression pattern of interferon regulated genes in the chicken.

作者信息

Röll Susanne, Härtle Stefan, Lütteke Thomas, Kaspers Bernd, Härtle Sonja

机构信息

Department for Veterinary Science, University of Munich, Munich, Germany.

formerly Department for Veterinary Science, University of Munich, Munich, Germany.

出版信息

BMC Genomics. 2017 Mar 28;18(1):264. doi: 10.1186/s12864-017-3641-6.

Abstract

BACKGROUND

Type I interferons are major players against viral infections and mediate their function by the induction of Interferon regulated genes (IRGs). Recently, it became obvious that these cytokines have a multitude of additional functions. Due to the unique features of the chickens' immune system, available data from mouse models are not easily transferable; hence we performed an extensive analysis of chicken IRGs.

RESULTS

A broad database search for homologues to described mammalian IRGs (common IRGs, cIRGs) was combined with a transcriptome analysis of spleen and lung at different time points after application of IFNα. To apply physiological amounts of IFN, half-life of IFN in the chicken was determined. Interestingly, the calculated 36 min are considerably shorter than the ones obtained for human and mouse. Microarray analysis revealed many additional IRGs (newly identified IRGs; nIRGs) and network analysis for selected IRGs showed a broad interaction of nIRGs among each other and with cIRGs. We found that IRGs exhibit a highly tissue and time specific expression pattern as expression quality and quantity differed strongly between spleen and lung and over time. While in the spleen for many affected genes changes in RNA abundance peaked already after 3 h, an increasing or plateau-like regulation after 3, 6 and 9 h was observed in the lung.

CONCLUSIONS

The induction or suppression of IRGs in chickens is both tissue and time specific and beside known antiviral mechanisms type I IFN induces many additional cellular functions. We confirmed many known IRGs and established a multitude of so far undescribed ones, thus providing a large database for future research on antiviral mechanisms and additional IFN functions in non-mammalian species.

摘要

背景

I型干扰素是对抗病毒感染的主要因子,并通过诱导干扰素调节基因(IRGs)来介导其功能。最近,很明显这些细胞因子具有多种其他功能。由于鸡免疫系统的独特特征,来自小鼠模型的现有数据不易转移;因此,我们对鸡IRGs进行了广泛分析。

结果

对已描述的哺乳动物IRGs(常见IRGs,cIRGs)的同源物进行广泛的数据库搜索,并结合在应用IFNα后不同时间点对脾脏和肺的转录组分析。为了应用生理量的IFN,测定了IFN在鸡体内的半衰期。有趣的是,计算得出的36分钟明显短于在人和小鼠中获得的半衰期。微阵列分析揭示了许多额外的IRGs(新鉴定的IRGs;nIRGs),对选定IRGs的网络分析表明nIRGs之间以及与cIRGs之间存在广泛的相互作用。我们发现IRGs表现出高度的组织和时间特异性表达模式,因为脾脏和肺之间以及随时间推移,表达质量和数量差异很大。在脾脏中,许多受影响基因的RNA丰度变化在3小时后已经达到峰值,而在肺中,在3、6和9小时后观察到增加或平台样调节。

结论

鸡体内IRGs的诱导或抑制具有组织和时间特异性,并且除了已知的抗病毒机制外,I型干扰素还诱导许多其他细胞功能。我们确认了许多已知的IRGs,并建立了许多迄今为止未描述的IRGs,从而为未来研究非哺乳动物物种的抗病毒机制和干扰素的其他功能提供了一个大型数据库。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5704/5371264/47e6e3d8ee53/12864_2017_3641_Fig1_HTML.jpg

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