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首页> 外文期刊>Nucleic acids research >Characterization of the structure and regulation of the murine gene encoding gut-enriched Krüppel-like factor (Krüppel-like factor 4)
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Characterization of the structure and regulation of the murine gene encoding gut-enriched Krüppel-like factor (Krüppel-like factor 4)

机译:编码富含肠道的Krüppel样因子(Krüppel样因子4)的鼠基因的结构和调控特性

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Gut-enriched Krüppel-like factor (GKLF, KLF4) is an epithelial-specific transcription factor whose expression is associated with growth arrest. In order to understand the mechanisms regulating expression of the gene encoding GKLF, we isolated a genomic clone containing murine GKLF. The gene spans 5.3 kb and contains four exons. A major start site of transcription was mapped to an adenine residue 601 nt 5′ of the translation initiation codon. An additional 1 kb of the 5′-flanking region was sequenced and found to contain multiple cis-elements homologous to the binding sites of several established transcription factors including Sp1, AP-1, Cdx, GATA, and USF. In particular, three closely spaced GC-boxes 5′ of the TATA box resemble the established binding site for GKLF. DNase I protection and electrophoretic mobility shift assays verified that recombinant GKLF bound to each of the three GC-boxes. In co-transfection experiments, GKLF transactivated a reporter gene linked to the GKLF1 kb 5′-flanking region, as did Sp1, Sp3 and Cdx-2. Mutations of one or both of the first and second GC-boxes in the promoter resulted in diminished transactivation by GKLF. These results demonstrate that the 5′-flanking sequence of the mouse GKLF gene functions as a promoter and is subject to autoregulation by its own gene product.
机译:富含肠道的Krüppel样因子(GKLF,KLF4)是一种上皮特异性转录因子,其表达与生长停滞有关。为了了解调节编码GKLF的基因表达的机制,我们分离了包含鼠GKLF的基因组克隆。该基因跨度5.3 kb,包含四个外显子。转录的主要起始位点被定位到翻译起始密码子的腺嘌呤残基601nt 5'。对另外的1kb的5'-侧翼区进行测序,发现其包含与多个已建立的转录因子(包括Sp1,AP-1,Cdx,GATA和USF)的结合位点同源的多个顺式元件。特别地,TATA盒的三个紧密间隔的GC盒5'类似于已建立的GKLF结合位点。 DNase I保护和电泳迁移率变动分析验证了重组GKLF与三个GC-box的每个结合。在共转染实验中,GKLF与Sp1,Sp3和Cdx-2一样,使与GKLF1 kb 5'侧翼区域相连的报告基因转活化。启动子中第一个和第二个GC盒中一个或两个的突变导致GKLF的反式激活减少。这些结果表明,小鼠GKLF基因的5'侧翼序列起启动子的作用,并通过其自身的基因产物进行自动调节。

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