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Cytokine-Induced Monocyte Characteristics in SLE

机译:SLE中细胞因子诱导的单核细胞特征

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摘要

Monocytes in SLE have been described as having aberrant behavior in a number of assays. We examined gene expression and used a genome-wide approach to study the posttranslational histone mark, H4 acetylation, to examine epigenetic changes in SLE monocytes. We compared SLE monocyte gene expression and H4 acetylation with three types of cytokine-treated monocytes to understand which cytokine effects predominated in SLE monocytes. We found that γ-interferon and α-interferon both replicated a broad range of the gene expression changes seen in SLE monocytes. H4 acetylation in SLE monocytes was overall higher than in controls and there was less correlation of H4ac with cytokine-treated cells than when gene expression was compared. A set of chemokine genes had downregulated expression and H4ac. Therefore, there are significant clusters of aberrantly expressed genes in SLE which are strongly associated with altered H4ac, suggesting that these cells have experienced durable changes to their epigenome.
机译:在许多分析中,SLE中的单核细胞被描述为具有异常行为。我们检查了基因表达并使用了全基因组方法来研究翻译后组蛋白标记H4乙酰化,以检查SLE单核细胞的表观遗传学变化。我们将SLE单核细胞基因表达和H4乙酰化与三种类型的经细胞因子处理的单核细胞进行了比较,以了解SLE单核细胞中哪种细胞因子效应占主导。我们发现γ-干扰素和α-干扰素都复制了在SLE单核细胞中看到的广泛的基因表达变化。与比较基因表达时相比,SLE单核细胞中的H4乙酰化总体上高于对照组,并且H4ac与经细胞因子处理的细胞的相关性较小。一组趋化因子基因下调了表达和H4ac。因此,SLE中有大量异常表达的基因簇,它们与H4ac的改变密切相关,表明这些细胞的表观基因组经历了持久的变化。

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