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首页> 外文期刊>Molecular and Cellular Biology >Structure and regulation of the human interferon regulatory factor 1 (IRF-1) and IRF-2 genes: implications for a gene network in the interferon system.
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Structure and regulation of the human interferon regulatory factor 1 (IRF-1) and IRF-2 genes: implications for a gene network in the interferon system.

机译:人类干扰素调节因子1(IRF-1)和IRF-2基因的结构和调控:对干扰素系统中基因网络的影响。

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Interferon regulatory factor 1 (IRF-1) and IRF-2 are structurally similar DNA-binding factors which were originally identified as regulators of the type I interferon (IFN) system; the former functions as a transcriptional activator, and the latter represses IRF-1 function by competing for the same cis elements. More recent studies have revealed new roles of the two factors in the regulation of cell growth; IRF-1 and IRF-2 manifest antioncogenic and oncogenic activities, respectively. In this study, we determined the structures and chromosomal locations of the human IRF-1 and IRF-2 genes and further characterized the promoters of the respective genes. Comparison of exon-intron organization of the two genes revealed a common evolutionary structure, notably within the exons encoding the N-terminal portions of the two factors. We confirmed the chromosomal mapping of the human IRF-1 gene to 5q31.1 and newly assigned the IRF-2 gene to 4q35.1, using fluorescence in situ hybridization. The 5' regulatory regions of both genes contain highly GC-rich sequences and consensus binding sequences for several known transcription factors, including NF-kappa B. Interestingly, one IRF binding site was found within the IRF-2 promoter, and expression of the IRF-2 gene was affected by both transient and stable IRF-1 expression. In addition, one potential IFN-gamma-activated sequence was found within the IRF-1 promoter. Thus, these results may shed light on the complex gene network involved in regulation of the IFN system.
机译:干扰素调节因子1(IRF-1)和IRF-2是结构相似的DNA结合因子,最初被确定为I型干扰素(IFN)系统的调节剂。前者起着转录激活剂的作用,而后者通过竞争相同的顺式元件来抑制IRF-1的功能。最近的研究揭示了这两个因素在调节细胞生长中的新作用。 IRF-1和IRF-2分别显示出抗癌活性和致癌活性。在这项研究中,我们确定了人类IRF-1和IRF-2基因的结构和染色体位置,并进一步表征了各个基因的启动子。比较两个基因的外显子-内含子组织发现一个共同的进化结构,特别是在编码这两个因子的N-末端部分的外显子内。我们证实了使用荧光原位杂交技术将人IRF-1基因的染色体定位为5q31.1,并将IRF-2基因新分配为4q35.1。这两个基因的5'调控区均含有高度GC丰富的序列和包括NF-κB在内的几种已知转录因子的共有结合序列。有趣的是,在IRF-2启动子中发现了一个IRF结合位点,并表达了IRF -2基因受瞬时和稳定IRF-1表达的影响。另外,在IRF-1启动子内发现了一种潜在的IFN-γ激活序列。因此,这些结果可能为干扰素系统调控所涉及的复杂基因网络提供了启示。

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