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在大多数细胞中,两个与DNA结合的E2二聚体对于强大的转录激活以及与细胞因子的协同作用是必需的。

Two DNA-bound E2 dimers are required for strong transcriptional activation and for cooperation with cellular factors in most cells.

作者信息

Gauthier J M, Dostatni N, Lusky M, Yaniv M

机构信息

Département des Biotechnologies, UA 1149 du Centre National de la Recherche Scientifique, Institut Pasteur, Paris, France.

出版信息

New Biol. 1991 May;3(5):498-509.

PMID:1653009
Abstract

The E2 transcriptional activator encoded by papillomaviruses binds as a dimer to the palindromic sequence ACCGNNNNCGGT present in several copies in the viral genomes. We show that strong activation requires that a minimum of two E2 binding sites are actually occupied by the protein. Studies with constructs bearing two E2 sites separated by variable lengths of DNA showed that there is no stereospecific constraint for E2 homosynergy. The capacity of E2 to cooperate with cellular factors interacting with the promoter/enhancer sequences of the genomes of human papilloma virus types 16, 18, or 33 was further investigated. In epithelial cells, one E2 dimer could not cooperate with the AP1 complex, the glucocorticoid receptor, or the NF1/K factor, whereas several E2 dimers could. These results lead to the notion of the "functional E2 tetramer" as the unit for strong transcriptional activation by E2 and for cooperativity with other cellular factors in this process. Finally, our results suggest that activators such as E2 or the glucocorticoid receptor may interact with partially different targets in the transcriptional machinery.

摘要

乳头瘤病毒编码的E2转录激活因子以二聚体形式与病毒基因组中多个拷贝存在的回文序列ACCGNNNNCGGT结合。我们发现,强烈的激活作用要求至少有两个E2结合位点被该蛋白实际占据。对带有两个被不同长度DNA隔开的E2位点的构建体进行的研究表明,E2同型协同作用不存在立体特异性限制。我们进一步研究了E2与与人乳头瘤病毒16型、18型或33型基因组的启动子/增强子序列相互作用的细胞因子协同作用的能力。在上皮细胞中,一个E2二聚体不能与AP1复合物、糖皮质激素受体或NF1/K因子协同作用,而几个E2二聚体则可以。这些结果引出了“功能性E2四聚体”这一概念,它是E2进行强烈转录激活以及在此过程中与其他细胞因子协同作用的单位。最后,我们的结果表明,诸如E2或糖皮质激素受体等激活因子可能与转录机制中的部分不同靶点相互作用。

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