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A Col9a1 enhancer element activated by two interdependent SOX9 dimers

机译:一个由两个相互依赖的SOX9二聚体激活的Col9a1增强子元件

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The transcription factor SOX9 plays a critical role in chondrogenesis as well as in sex determination. Previous work has suggested that SOX9 functions as a DNA-dependent dimer when it activates genes involved in chondrogenesis, but functions as a monomer to activate genes involved in sex determination. We present evidence herein for a third binding configuration through which SOX9 can activate transcription. We have identified four separate SOX consensus sequences in a COL9A1 collagen gene enhancer. The sites are arranged as two pairs, and each pair is similar to previously discovered dimeric SOX9 binding sites. Increasing the spacing between the pairs of sites eliminated enhancer activity in chondrocytic cells, as did the mutation of any one of the four sites. The COL9A1 enhancer is ordinarily inactive in 10T1/2 cells, but cotransfection with a SOX9 expression plasmid was sufficient to activate the enhancer, and mutation of any one of the four sites reduced responsiveness to SOX9 overexpression. These results suggest a novel mechanism for transcriptional activation by SOX9, in which two SOX9 dimers that are bound at the two pairs of sites are required to interact with one another, either directly or indirectly, in order to produce a functional transcriptional activation complex.
机译:转录因子SOX9在软骨形成以及性别确定中起着至关重要的作用。先前的工作表明,SOX9激活与软骨形成有关的基因时,会起DNA依赖性二聚体的作用,但会作为激活与性别决定有关的基因的单体而起作用。我们在这里为SOX9可以激活转录的第三种结合构型提供证据。我们在COL9A1胶原蛋白基因增强子中鉴定了四个单独的SOX共有序列。这些位点按两对排列,每对类似于以前发现的二聚体SOX9结合位点。增大位点对之间的间隔,消除了软骨细胞中的增强子活性,四个位点中任一位点的突变也是如此。通常,COL9A1增强子在10T1 / 2细胞中是无活性的,但是与SOX9表达质粒的共转染足以激活该增强子,并且四个位点中任何一个的突变都降低了对SOX9过表达的响应性。这些结果表明了一种通过SOX9进行转录激活的新机制,其中需要在两对位点结合的两个SOX9二聚体直接或间接相互作用,以产生功能性转录激活复合物。

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