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十二指肠转录组谱分析揭示硼补充对调节大鼠免疫活性的重要性。

Transcriptome Profiling of Duodenum Reveals the Importance of Boron Supplementation in Modulating Immune Activities in Rats.

机构信息

College of Animal Science, Anhui Science and Technology University, No. 9 Donghua Road, Fengyang County, Chuzhou, Anhui Province, China.

Anhui Province Key Laboratory of Animal Nutritional Regulation and Health, No. 9, Donghua Road, Fengyang County, Chuzhou, Anhui Province, China.

出版信息

Biol Trace Elem Res. 2022 Aug;200(8):3762-3773. doi: 10.1007/s12011-021-02983-w. Epub 2021 Nov 12.

Abstract

As an essential trace element, appropriate boron supplementation can promote immune function of animals. To illustrate the effects of boron in a rat model, RNA-Seq was conducted for the RNA from duodenum after treatment with different concentration of boron in which boron was given in the form of boric acid. More than 47 million reads were obtained in 0, 10, and 320 mg/L boron (0, 57.21, and 1830.66 mg/L boric acid) treatment groups that produced 58 965 402, 48 607 328, and 46 760 660 clean reads, respectively. More than 95% of the clean reads were successfully matched to the rat reference genome and assembled to generate 32 662 transcripts. A total of 624 and 391 differentially expressed candidate genes (DEGs) were found between 0 vs.10 and 0 vs. 320 mg/L boron comparison groups. We also identified transcription start site, transcription terminal site, and skipped exons as the main alternative splicing events. GO annotations revealed most of DEGs were involved in the regulation of immune activity. The DEGs were enriched in influenza A, herpes simplex infection, cytosolic DNA-sensing pathway, and antigen processing and presentation signaling pathways. The expression levels of genes enriched in these signaling pathways indicate that lower doses of boron could achieve better effects on promoting immune response in the duodenum. These effects on the immune system appear to be mediated via altering the expression patterns of genes involved in the related signaling pathways in a dose-dependent pattern. These data provide more insights into the molecular mechanisms of immune regulation in rats in response to dietary boron treatment.

摘要

作为一种必需的微量元素,适量的硼补充可以促进动物的免疫功能。为了说明硼在大鼠模型中的作用,我们对不同浓度硼处理后十二指肠的 RNA 进行了 RNA-Seq 分析,其中硼是以硼酸的形式给予的。在 0、10 和 320mg/L 硼(0、57.21 和 1830.66mg/L 硼酸)处理组中获得了超过 4700 万条读数,分别产生了 58965402、48607328 和 46760660 条清洁读数。超过 95%的清洁读数成功匹配了大鼠参考基因组,并组装生成 32662 个转录本。在 0 与 10mg/L 硼和 0 与 320mg/L 硼比较组之间,共发现了 624 个和 391 个差异表达候选基因(DEGs)。我们还鉴定了转录起始位点、转录末端位点和跳过外显子作为主要的可变剪接事件。GO 注释显示,大多数 DEGs 参与免疫活性的调节。DEGs 在流感 A、单纯疱疹感染、细胞质 DNA 感应途径和抗原加工和呈递信号通路中富集。这些信号通路中富集的基因的表达水平表明,较低剂量的硼可以在十二指肠中更好地促进免疫反应。这些对免疫系统的影响似乎是通过改变与相关信号通路相关的基因的表达模式,以剂量依赖的方式介导的。这些数据为饮食硼处理对大鼠免疫系统调节的分子机制提供了更多的见解。

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