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Asynchronous replication timing of imprinted loci is independent of DNA methylation but consistent with differential subnuclear localization

机译:印迹基因座的异步复制时间与DNA甲基化无关但与差异性亚核定位相一致

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摘要

Genomic imprinting in mammals marks the two parental alleles resulting in differential gene expression. Imprinted loci are characterized by distinct epigenetic modifications such as differential DNA methylation and asynchronous replication timing. To determine the role of DNA methylation in replication timing of imprinted loci, we analyzed replication timing in Dnmt1- and Dnmt3L-deficient embryonic stem (ES) cells, which lack differential DNA methylation and imprinted gene expression. Asynchronous replication is maintained in these ES cells, indicating that asynchronous replication is parent-specific without the requirement for differential DNA methylation. Imprinting centers are required for regional control of imprinted gene expression. Analysis of replication fork movement and three-dimensional RNA and DNA fluoroscent in situ hybridization (FISH) analysis of the Igf2-H19 locus in various cell types indicate that the Igf2-H19 imprinting center differentially regulates replication timing of nearby replicons and subnuclear localization. Based on these observations, we suggest a model in which cis elements containing nonmethylation imprints are responsible for the movement of parental imprinted loci to distinct nuclear compartments with different replication characteristics resulting in asynchronous replication timing.
机译:哺乳动物中的基因组印记标记了两个亲本等位基因,导致差异基因表达。印迹基因座的特征是独特的表观遗传修饰,例如差异DNA甲基化和异步复制时间。为了确定DNA甲基化在印迹基因座复制时间中的作用,我们分析了缺乏差异DNA甲基化和印迹基因表达的Dnmt1和Dnmt3L缺陷型胚胎干(ES)细胞中的复制时间。这些ES单元中维持异步复制,这表明异步复制是特定于父代的,而无需差异化的DNA甲基化。印迹中心对于印迹基因表达的区域控制是必需的。复制叉运动的分析以及在各种细胞类型中对Igf2-H19基因座进行的三维RNA和DNA荧光原位杂交(FISH)分析表明,Igf2-H19印迹中心差异性调节附近复制子的复制时间和亚核定位。基于这些观察结果,我们建议一个模型,其中包含非甲基化印记的顺式元件负责将亲本印记基因座移动到具有不同复制特性的不同核区室,从而导致异步复制时间。

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