首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Sea urchin early histone H2A modulator binding factor 1 is a positive transcription factor also for the early histone H3 gene.
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Sea urchin early histone H2A modulator binding factor 1 is a positive transcription factor also for the early histone H3 gene.

机译:海胆早期组蛋白H2A调节剂结合因子1也是早期组蛋白H3基因的正转录因子。

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摘要

To shed some light on the mechanisms involved in the coordinate regulation of the early histone gene set during sea urchin development, we tested the hypothesis that the upstream sequence element USE1, previously identified in the early H2A modulator, could also participate in the transcription of the early histone H3 gene. We found by DNAse I protection analysis and by competition in electrophoretic mobility-shift experiments that two sequence elements of the H3 promoter closely resembled the USE1-H2A sequence in their binding activity for nuclear factors from 64-cell stage embryos. These modulator binding factor 1 (MBF-1)-related factors seem to recognize the ACAGA motif that is conserved between the USE1-like sequences of both H2A and H3 promoters. In fact, excess oligonucleotide containing a mutated USE1-H2A element in which the ACAGA sequence was mutated to AGTCA failed to compete with the USE1 sites of both H2A and H3 genes for interaction with MBF-1. Finally, in vivo transcriptional analysis in both Xenopus and sea urchin showed that an excess of USE1-H2A element efficiently competed for the activity of the H3 promoter. From these results we conclude that MBF-1 is a transcription factor conserved between sea urchin and frog and that MBF-1 or related transcription factors are involved in the coordinate expression of both H2A and H3 early histone genes.
机译:为了阐明海胆发育过程中早期组蛋白基因集的协调调控所涉及的机制,我们测试了以下假设:先前在早期H2A调节剂中鉴定出的上游序列元件USE1也可以参与转录。早期组蛋白H3基因。我们通过DNAse I保护分析和电泳迁移率迁移实验的竞争发现,H3启动子的两个序列元件在与64细胞阶段胚胎的核因子结合活性方面与USE1-H2A序列极为相似。这些与调节剂结合因子1(MBF-1)相关的因子似乎识别了HCA和H3启动子的USE1样序列之间保守的ACAGA基序。实际上,过量的含有突变的USE1-H2A元件的寡核苷酸无法与H2A和H3基因的USE1位点竞争与MBF-1的相互作用,在该突变中,ACAGA序列被突变为AGTCA。最后,在非洲爪蟾和海胆中的体内转录分析表明,过量的USE1-H2A元件可有效竞争H3启动子的活性。从这些结果,我们得出结论,MBF-1是海胆和青蛙之间保守的转录因子,MBF-1或相关转录因子参与H2A和H3早期组蛋白基因的协调表达。

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