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Differential roles for MBD2 and MBD3 at methylated CpG islands, active promoters and binding to exon sequences

机译:MBD2和MBD3在甲基化CpG岛上的不同作用,活性启动子和与外显子序列的结合

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摘要

The heterogeneous collection of nucleosome remodelling and deacetylation (NuRD) complexes can be grouped into the MBD2- or MBD3-containing complexes MBD2–NuRD and MBD3–NuRD. MBD2 is known to bind to methylated CpG sequences in vitro in contrast to MBD3. Although functional differences have been described, a direct comparison of MBD2 and MBD3 in respect to genome-wide binding and function has been lacking. Here, we show that MBD2–NuRD, in contrast to MBD3–NuRD, converts open chromatin with euchromatic histone modifications into tightly compacted chromatin with repressive histone marks. Genome-wide, a strong enrichment for MBD2 at methylated CpG sequences is found, whereas CpGs bound by MBD3 are devoid of methylation. MBD2-bound genes are generally lower expressed as compared with MBD3-bound genes. When depleting cells for MBD2, the MBD2-bound genes increase their activity, whereas MBD2 plus MBD3-bound genes reduce their activity. Most strikingly, MBD3 is enriched at active promoters, whereas MBD2 is bound at methylated promoters and enriched at exon sequences of active genes.
机译:核小体重塑和去乙酰化(NuRD)复合物的异质集合可分为包含MBD2-或MBD3的复合物MBD2-NuRD和MBD3-NuRD。与MBD3相反,已知MBD2在体外与甲基化CpG序列结合。尽管已经描述了功能上的差异,但是仍缺乏将MBD2和MBD3就全基因组结合和功能进行直接比较的方法。在这里,我们显示MBD2-NuRD与MBD3-NuRD相比,将常染色质组蛋白修饰的开放染色质转化为具有压迫性组蛋白标记的紧密染色质。在全基因组范围内,发现在甲基化的CpG序列中MBD2有很强的富集,而与MBD3结合的CpG没有甲基化。与结合MBD3的基因相比,结合MBD2的基因通常表达较低。当耗尽细胞中的MBD2时,MBD2结合的基因会增加其活性,而MBD2加MBD3的结合基因会降低其活性。最引人注目的是,MBD3在活性启动子上富集,而MBD2在甲基化启动子上结合,并在活性基因的外显子序列上富集。

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