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Echinacea purpurea (L.) Moench treatment of monocytes promotes tonic interferon signaling, increased innate immunity gene expression and DNA repeat hypermethylated silencing of endogenous retroviral sequences

机译:紫外线紫癜(L.)单核细胞的烟雾处理促进滋补干扰素信号传导,增加先天免疫基因表达和DNA重复内源性逆转录病毒序列的超甲基化沉默

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Herbal remedies of Echinacea purpurea tinctures are widely used today to reduce common cold respiratory tract infections. Transcriptome, epigenome and kinome profiling allowed a systems biology level characterisation of genomewide immunomodulatory effects of a standardized Echinacea purpurea (L.) Moench extract in THP1 monocytes. Gene expression and DNA methylation analysis revealed that Echinaforce? treatment triggers antiviral innate immunity pathways, involving tonic IFN signaling, activation of pattern recognition receptors, chemotaxis and immunometabolism. Furthermore, phosphopeptide based kinome activity profiling and pharmacological inhibitor experiments with filgotinib confirm a key role for Janus Kinase (JAK)-1 dependent gene expression changes in innate immune signaling. Finally, Echinaforce? treatment induces DNA hypermethylation at intergenic CpG, long/short interspersed nuclear DNA repeat elements (LINE, SINE) or long termininal DNA repeats (LTR). This changes transcription of flanking endogenous retroviral sequences (HERVs), involved in an evolutionary conserved (epi) genomic protective response against viral infections. Altogether, our results suggest that Echinaforce? phytochemicals strengthen antiviral innate immunity through tonic IFN regulation of pattern recognition and chemokine gene expression and DNA repeat hypermethylated silencing of HERVs in monocytes. These results suggest that immunomodulation by Echinaforce? treatment holds promise to reduce symptoms and duration of infection episodes of common cold corona viruses (CoV), Severe Acute Respiratory Syndrome (SARS)-CoV, and new occurring strains such as SARS-CoV-2, with strongly impaired interferon (IFN) response and weak innate antiviral defense.
机译:目前,海胆紫癜酊的草药补救措施是广泛应用的,以减少常见的冷呼吸道感染。转录组,外延蛋白酶和Kinome分析允许系统生物学水平表征在THP1单核细胞中标准化的海胆紫癜(L.)Moench提取物的基因微调免疫调节作用。基因表达和DNA甲基化分析显示EchinaForce?治疗触发抗病毒先天免疫途径,涉及滋补IFN信号,模式识别受体,趋化性和免疫法的激活。此外,基于磷酸肽的Kinome活性分析和药理学抑制剂实验与Filgotinib的实验证实了Janus激酶(Jak)-1依赖性基因表达的关键作用是先天免疫信号传导的变化。最后,EchinaForce?治疗在非基因CpG中诱导DNA高甲基化,长/短孔核DNA重复元素(线,正弦)或长末端DNA重复(LTR)。这种改变了侧翼内源性逆转录病毒序列(HERV)的转录,参与了对病毒感染的进化保守(EPI)基因组保护响应。完全是,我们的结果表明EchinaForce?植物化学术通过滋补IFN调节模式识别和趋化因子基因表达和DNA重复单核细胞中腰蛋白的抗病毒先天免疫。这些结果表明EchinaForce的免疫调节?治疗持希望减少普通冷电晕病毒(COV),严重急性呼吸综合征(SARS)-CoV的感染发作的症状和持续时间,以及SARS-COV-2的新发生菌株,具有较大受损的干扰素(IFN)反应和弱天生的抗病毒防御。

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