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Regulation of gene expression in mast cells: micro-RNA expression and chromatin structural analysis of cytokine genes

机译:肥大细胞中基因表达的调节:细胞因子基因的微RNA表达和染色质结构分析

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Despite deriving from two different compartments of the immune system (myeloid and lymphoid respectively), Th2 cells and mast cells produce the same panel of cytokines, interleukin (IL)4, IL5 and IL13. We have compared the chromatin structure of the RAD50/ IL13/ILA locus in Th2 cells and mast cells. Th2 and mast cells display strong overlap in their patterns of DNase I hypersensitivity throughout this locus, except that the first intron of the IL13 gene (MCHS) is DNase I hypersensitive only in mast cells and the conserved non-coding sequence (CNS)-1 in the IL4/IL13 intergenic region is DNase I hypersensitive only in Th2 cells (explaining why cytokine expression is impaired in Th2 cells but not in mast cells of CNS-1-deleted mice). We have also examined the role of micro-RNAs (miRNAs) in the development and activation of mast cells and T cells. miRNAs are 21- to 25-nucleotide small RNAs that regulate gene expression post-transcriptionally by targeting protein-coding mRNAs. Using oligonucleotide arrays to analyse miRNA expression in murine T cells and mast cells, we have identified distinctive cell type-specific patterns of miRNA expression as well as changes related to differentiation and cell activation. We are studying the biological functions of selected miRNAs.
机译:尽管从免疫系统的两个不同隔室(分别分别是髓样和淋巴管),但TH2细胞和肥大细胞产生相同的细胞因子,白细胞介素(IL)4,IL5和IL13。我们在TH2细胞和肥大细胞中比较了RAD50 / IL13 / ILA基因座的染色质结构。除了IL13基因(MCH)的第一个内含子之外,TH2和肥大细胞在整个轨迹中显示出强烈的重叠在整个基因座中,除了IL13基因(MCH)的第一个内含子仅在肥大细胞和保守的非编码序列(CNS)-1中仅过敏在IL4 / IL13中,基因因子是DNA酶I仅在TH2细胞中过敏(解释为什么细胞因子表达在TH2细胞中损害,但不在CNS-1缺失小鼠的肥大细胞中)。我们还研究了微RNA(miRNA)在肥大细胞和T细胞的开发和激活中的作用。 MiRNA是21至25核苷酸小RNA,其通过靶向蛋白质编码MRNA来调节转录的基因表达。使用寡核苷酸阵列分析小鼠T细胞和肥大细胞中的miRNA表达,我们已经确定了miRNA表达的独特细胞类型特异性模式以及与分化和细胞活化有关的变化。我们正在研究所选miRNA的生物学功能。

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