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首页> 外文期刊>Nucleic Acids Research >Oct-2 regulates CD36 gene expression via a consensus octamer, which excludes the co-activator OBF-1
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Oct-2 regulates CD36 gene expression via a consensus octamer, which excludes the co-activator OBF-1

机译:Oct-2通过共有八聚体调节CD36基因表达,该共聚八聚体排除了共激活因子OBF-1

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摘要

The POU domain transcription factor, Oct-2, is essential for the B cell-specific expression of CD36 in mouse B cells. In order to determine how Oct-2 mediates expression of CD36 in B cells, we cloned and analysed the mouse CD36 promoter. In contrast to the human CD36 promoter, the mouse promoter contains a consensus octamer element of the type ATGCTAAT. This cotamer element can be bound by either Oct-1 or Oct-2 but requires the expression of Oct-2 to activate transcription in B cells. Mutation of the octamer element renders the CD36 promoter refractory to activation by Oct-2. Furthermore, we demonstrate that the CD36 octamer element does not support recruitment of the B cell-specific co-activator OBF-1 and that CD36 expression is unaffected in primary B cells derived from obf-1~(-1-) mice. We conclude that Oct-2 activates CD36 gene expression in mouse B cells via the octamer element in the promoter. Our data also demonstrate that CD36 is the first example of an Oct-2-dependent gene whose expression in B cells is independent of OBF-1. These findings support the notion that Oct-2 regulates gene transcription by both OBF-1-dependent and -independent mechanisms.
机译:POU域转录因子Oct-2对于小鼠B细胞中CD36的B细胞特异性表达至关重要。为了确定Oct-2如何介导B细胞中CD36的表达,我们克隆并分析了小鼠CD36启动子。与人CD36启动子相反,小鼠启动子包含ATGCTAAT类型的共有八聚体元件。此共聚物元素可以与Oct-1或Oct-2结合,但需要表达Oct-2才能激活B细胞中的转录。八聚体元件的突变使CD36启动子难以被Oct-2激活。此外,我们证明了CD36八聚体元素不支持B细胞特异性共激活因子OBF-1的募集,并且CD36的表达在源自obf-1〜(-1-)小鼠的原代B细胞中不受影响。我们得出结论,Oct-2通过启动子中的八聚体元素激活小鼠B细胞中的CD36基因表达。我们的数据还证明CD36是Oct-2依赖基因的第一个例子,该基因在B细胞中的表达独立于OBF-1。这些发现支持了Oct-2通过OBF-1依赖性和非依赖性机制调节基因转录的观点。

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