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Binding sites in mammalian genes and viral gene regulatory regions recognized by methylated DNA-binding protein.

机译:甲基化DNA结合蛋白识别的哺乳动物基因和病毒基因调节区中的结合位点。

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摘要

Methylated DNA-binding protein (MDBP), a ubiquitous mammalian protein, recognizes a variety of related DNA sequences. Some of these sequences require methylation of their CpG dinucleotides for binding and others do not. We report that MDBP binds, in a DNA methylation-independent fashion, to two sites in the mouse polyomavirus enhancer, one in the enhancer of the human hepatitis B virus, and to one in the long terminal repeat of equine infectious anemia proviral DNA. We have also found a number of MDBP sites in human and rodent DNAs which bind much better to MDBP when they are methylated at CpG dinucleotides within the recognition site. These include sites at the beginning of the human genes for hypoxanthine phosphoribosyl transferase, HLA-A2, -A3, and -A25 antigens, and alpha-galactosidase A. In the case of methylation-responsive MDBP sites, changes in their methylation status during differentiation or DNA replication could help drive development by modulating transcription.
机译:甲基化的DNA结合蛋白(MDBP)是一种普遍存在的哺乳动物蛋白,可识别多种相关的DNA序列。这些序列中的一些需要其CpG二核苷酸的甲基化才能结合,而其他序列则不需要。我们报告说,MDBP以DNA甲基化独立的方式结合到小鼠多瘤病毒增强子中的两个位点,一个在人类乙型肝炎病毒的增强子中,和一个在马传染性贫血前病毒DNA的长末端重复序列中。我们还发现了人和啮齿动物DNA中的许多MDBP位点,当它们在识别位点的CpG二核苷酸处甲基化时,它们与MDBP的结合更好。这些包括在人类基因的次黄嘌呤磷酸核糖基转移酶,HLA-A2,-A3和-A25抗原以及α-半乳糖苷酶A的位点。对于甲基化反应性MDBP位点,在分化过程中其甲基化状态会发生变化DNA复制可以通过调节转录来帮助促进发育。

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