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首页> 外文期刊>The Journal of biological chemistry >Dispersed Chromosomal Stat5b-binding Elements Mediate Growth Hormone-activated Insulin-like Growth Factor-I Gene Transcription
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Dispersed Chromosomal Stat5b-binding Elements Mediate Growth Hormone-activated Insulin-like Growth Factor-I Gene Transcription

机译:分散的染色体Stat5b结合元素介导生长激素活化的胰岛素样生长因子-i基因转录

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摘要

The growth hormone (GH)-insulin-like growth factor-I (IGF-I) axis regulates somatic growth during childhood and orchestrates tissue repair throughout the life span. Recently described inactivating mutations in Stat5b in humans with impaired growth have focused attention on this transcription factor as a key agent linking GH-stimulated signals to IGF-I gene expression, and several putative Stat5b sites have been identified in the IGF-I gene. Here, we define and characterize potential GH- and Stat5b-activated chromosomal enhancers that can regulate IGF-I gene transcription. Of 89 recognizable Stat5 sequences in 200 kb centering on the rat IGF-I gene, 22 resided within conserved regions and/or were identical among different species. Only 15 of these sites, organized into 7 distinct domains, were found to bind Stat5b by quantitative chromatin immunoprecipitation assays in liver chromatin of rats, but only after acute GH treatment. These sites could bind Stat5b in vitro, and individual domains could mediate GH- and Stat5b-stimulated IGF-I promoter activity in cultured cells. Further analyses revealed that four Stat5b domains possessed chromatin signatures of enhancers, including binding of co-activators p300 and Med1, and RNA polymerase II. These modifications preceded GH-stimulated recruitment of Stat5b, as did lysine 4 monomethylation of histone H3, which was enriched in 6/7 Stat5b-binding elements. In contrast, histone acetylation was induced by GH but was limited to Stat5b binding domains found within the IGF-I transcription unit. We conclude that GH stimulates recruitment of Stat5b to multiple dispersed regions within the igf1 locus, including several with properties consistent with long range transcriptional enhancers that collectively regulate GH-activated IGF-I gene transcription.
机译:生长激素(GH) - 胰岛素样生长因子-i(IGF-1)轴调节儿童时期的体细胞生长,并在整个寿命中策划组织修复。最近描述了具有受损生长受损的人类中的Stat5B中的灭活突变对该转录因子的关注重点是将GH刺激的信号与IGF-I基因表达的关键剂联系起来,并且在IGF-I基因中鉴定了几个推定的STAT5B位点。在这里,我们定义和表征可以调节IGF-I基因转录的潜在的GH-和Stat5B激活的染色体增强剂。在89个可识别的STAT5序列中,在大鼠IGF-I基因上以200kb为中心,22例居住在保守区域内和/或在不同物种中相同。在大鼠肝脏染色质的定量染色质免疫沉淀测定中发现,这些位点中只有15个组织成7个不同的结构域,但仅在急性GH治疗后才能结合STAT5B。这些位点可以在体外结合STAT5B,并且个体结构域可以在培养细胞中介导GH-和Stat5B刺激的IGF-I启动子活性。进一步分析显示,四个STAT5B结构域具有增强剂的染色蛋白特征,包括共激活剂P300和MED1的结合,以及RNA聚合酶II。这些修改之前的GH刺激的STAT5B的募集,如组蛋白H3的赖氨酸4单甲基化,其富含6/7 Stat5B结合元素。相反,通过GH诱导组蛋白乙酰化,但仅限于IGF-I转录单元中发现的Stat5B结合域。我们得出结论,GH刺激STAT5B对IGF1基因座内的多个分散区域的募集,包括几种与长距离转录增强剂一致的特性,所述长距重转录增强剂共同调节GH激活的IGF-I基因转录。

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