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首页> 外文期刊>Molecular and Cellular Biology >Interaction between NF-kappa B- and serum response factor-binding elements activates an interleukin-2 receptor alpha-chain enhancer specifically in T lymphocytes.
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Interaction between NF-kappa B- and serum response factor-binding elements activates an interleukin-2 receptor alpha-chain enhancer specifically in T lymphocytes.

机译:NF-κB和血清反应因子结合元件之间的相互作用可特异性激活T淋巴细胞中的白介素2受体α链增强剂。

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We find that a short enhancer element containing the NF-kappa B binding site from the interleukin-2 receptor alpha-chain gene (IL-2R alpha) is preferentially activated in T cells. The IL-2R alpha enhancer binds NF-kappa B poorly and is only weakly activated by the NF-kappa B site alone. Serum response factor (SRF) binds to a site adjacent to the NF-kappa B site in the IL-2R enhancer, and both sites together have strong transcriptional activity specifically in T cells. Surprisingly, the levels of SRF constitutively expressed in T cells are consistently higher than in other cell types. Overexpression of SRF in B cells causes the IL-2R enhancer to function as well as it does in T cells, suggesting that the high level of SRF binding in T cells is functionally important.
机译:我们发现,包含来自白介素2受体α-链基因(IL-2Rα)的NF-κB结合位点的短增强子元件在T细胞中被优先激活。 IL-2Rα增强剂与NF-κB的结合较弱,仅被NF-κB部位弱激活。血清反应因子(SRF)与IL-2R增强子中与NF-κB位点相邻的位点结合,并且这两个位点在一起特别在T细胞中具有很强的转录活性。令人惊讶地,在T细胞中组成性表达的SRF水平始终高于其他细胞类型。 B细胞中SRF的过表达导致IL-2R增强子的功能与T细胞中的相同,这表明T细胞中SRF的高水平结合在功能上很重要。

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