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The NFAT-1 DNA binding complex in activated T cells contains Fra-1 and JunB.

机译：活化的T细胞中的NFAT-1 DNA结合复合物包含Fra-1和JunB。

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Activation of T cells induces transcription of the interleukin-2 (IL-2) gene. IL-2 expression is regulated through the binding of transcription factors to multiple sites within the IL-2 enhancer. One such cis-acting element within the IL-2 enhancer is the NFAT-1 (nuclear factor of activated T cells) binding site. NFAT-1 binding activity is absent in resting cells but is induced upon T-cell activation. The induction of NFAT-1 binding activity can be inhibited by cyclosporin A, potentially accounting for the ability of cyclosporin A to inhibit IL-2 production by T cells. We have previously reported that the NFAT-1 binding complex is composed of at least two proteins and that the 5' portion of the NFAT-1 sequence acts as a binding site for one or more proteins from the Ets family of transcription factors. We now report that the 3' portion of the NFAT-1 sequence contains a variant AP-1 binding site. NFAT-1 binding can be specifically inhibited by oligonucleotides containing a consensus AP-1 site. Moreover, mutation of the AP-1 site at the 3' end of the NFAT-1 sequence inhibits both NFAT-1 binding and the ability of the NFAT-1 binding site to activate expression from a reporter plasmid upon T-cell activation. Since AP-1 sites bind dimeric protein complexes composed of individual members of the Fos and Jun families of transcription factors, we used antibodies specific for individual Fos and Jun family members to determine whether they are present in the NFAT-1 binding complex. These experiments demonstrated that the NFAT-1 binding complex contains JunB and Fra-1 proteins. Northern (RNA) blot analyses demonstrate that both fra-1 and junB mRNAs are induced upon T-cell activation, although fra-1 mRNA is present even in quiescent T cells. Of interest, junB is not expressed in quiescent T cells, and it is induced with kinetics that are similar to those for the induction of IL-2 mRNA expression. Taken together, these results suggested that the JunB-Fra-1 heterodimer is the inducible nuclear component of the NFAT-1 binding activity and that JunB expression regulates the formation of the heterodimer. In addition, these data indicated that specific heterodimers of Fos and Jun family members may have selective roles in the induction of transcription during cellular activation.

机译：T细胞的激活诱导白介素2（IL-2）基因的转录。 IL-2表达通过转录因子与IL-2增强子内多个位点的结合来调节。 IL-2增强子中的一种此类顺式作用元件是NFAT-1（活化T细胞的核因子）结合位点。 NFAT-1结合活性在静止细胞中不存在，但在T细胞活化后被诱导。 NFAT-1结合活性的诱导可以被环孢菌素A抑制，这可能解释了环孢菌素A抑制T细胞产生IL-2的能力。我们以前曾报道过NFAT-1结合复合物由至少两种蛋白质组成，并且NFAT-1序列的5'部分充当一种或多种来自Ets转录因子家族蛋白质的结合位点。现在我们报告NFAT-1序列的3'部分包含一个变体AP-1结合位点。 NFAT-1结合可以被含有共有AP-1位点的寡核苷酸特异性抑制。此外，在NFAT-1序列3'端的AP-1位点发生突变，既抑制了NFAT-1结合，又抑制了NFAT-1结合位点激活T细胞活化后从报告质粒表达的能力。由于AP-1位点结合了由转录因子Fos和Jun家族的各个成员组成的二聚体蛋白复合物，因此我们使用了针对Fos和Jun家族的个体特异性的抗体来确定它们是否存在于NFAT-1结合复合物中。这些实验表明，NFAT-1结合复合物包含JunB和Fra-1蛋白。 Northern（RNA）印迹分析表明，尽管fra-1 mRNA即使在静止的T细胞中也存在，但fra-1和junB mRNA均在T细胞活化后被诱导。有趣的是，junB在静止的T细胞中不表达，它的诱导动力学与诱导IL-2 mRNA表达的动力学相似。综上所述，这些结果表明，JunB-Fra-1异二聚体是NFAT-1结合活性的可诱导核成分，并且JunB表达调节异二聚体的形成。此外，这些数据表明，Fos和Jun家族成员的特定异二聚体可能在细胞激活过程中的转录诱导中具有选择性作用。

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Boise, L H; Petryniak, B; Mao, X; June, C H; Wang, C Y; Lindsten, T; Bravo, R; Kovary, K; Leiden, J M; Thompson, C B;
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年度 1993
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专利

1. The NFAT-1 DNA binding complex in activated T cells contains Fra-1 and JunB. [J] . L H Boise, B Petryniak, X Mao, Molecular and Cellular Biology . 1993,第3期

机译：活化的T细胞中的NFAT-1 DNA结合复合物包含Fra-1和JunB。
2. Tumor promotion resistant cells are deficient in AP-1 DNA binding, JunD DNA binding and JunD expression and form different AP-1-DNA complexes than promotion sensitive cells. [J] . Bernstein LR, Walker SE Biochimica et biophysica acta: international journal of biochemistry and biophysics . 1999,第2a3期

机译：抗肿瘤促进细胞与促进敏感细胞相比，AP-1 DNA结合，JunD DNA结合和JunD表达不足，并且形成不同的AP-1-DNA复合物。
3. Predominant expression of nuclear activator protein-1 complex with DNA binding activity following systemic administration of N-methyl-D-aspartate in dentate granule cells of murine hippocampus. [J] . Yoneda Y, Ogita K, Azuma Y, Neuroscience: An International Journal under the Editorial Direction of IBRO . 1999,第1期

机译：在鼠海马齿状颗粒细胞中全身施用N-甲基-D-天冬氨酸后，核激活蛋白1复合物的主要表达具有DNA结合活性。
4. HDX Reveals DNA Binding Modulates Ligand-dependent Co-activator Interaction with the VDR/RXR Nuclear Receptor Complex [C] . Jun Zhang, Michael J. Chalmers, Keith R. Stayrook, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2010

机译：HDX显示DNA结合调节与VDR / RXR核受体复合物的配体依赖性共激活物相互作用
5. Dissecting the Mechanism of Arp2/3 Complex Activation by Actin Filament Binding and the Regulation and Function of JMY in Cells. [D] . Firat, Elif Nur. 2010

机译：剖析肌动蛋白丝结合Arp2 / 3复合物激活的机制以及细胞中JMY的调控和功能。
6. The NFAT-1 DNA binding complex in activated T cells contains Fra-1 and JunB. [O] . L H Boise, B Petryniak, X Mao, 1993

机译：活化的T细胞中的NFAT-1 DNA结合复合物包含Fra-1和JunB。
7. High glucose-induced DNA-binding activities of nuclear factor of activated T cells 5 and carbohydrate response element binding protein to the myo-inositol oxygenase gene are inhibited by sorbinil in peripheral blood mononuclear cells from patients with type 1 diabetes mellitus and nephropathy [O] . Yang Bingmei, Hodgkinson Andrea, Millward Beverley A., 2010

机译：山梨醇可抑制1型糖尿病和肾病患者外周血单个核细胞中高糖诱导的活化T细胞5核因子的DNA结合活性以及糖基化反应因子结合蛋白与肌醇加氧酶基因的结合。
8. NFAT-1 DNA Binding Complex in Activated T Cells Contains Fra-1 and JunB [R] . Boise, L. H., Petryniak, B., Mao, X., 1993

机译：活化T细胞中的NFaT-1 DNa结合复合物含有Fra-1和JunB

The NFAT-1 DNA binding complex in activated T cells contains Fra-1 and JunB.

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