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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >An upstream insulator regulates DLK1 imprinting in AML.
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An upstream insulator regulates DLK1 imprinting in AML.

机译:上游绝缘体调节AML中的DLK1印迹。

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摘要

DLK1 is an imprinted gene on chromosome 14. Using informative coding single nucleotide polymorphisms, we found DLK1 expression to be monoallelic in normal bone marrow, whereas it was biallelic in 76% of acute myeloid leukemia (AML) overexpressing DLK1 (61% of all AML). Quantitative methylation analysis of 7 cytosine-phosphate-guanosine-rich areas (3 upstream of or within DLK1, the putative intergenic-differentially methylated region and 3 upstream of or within MEG3) revealed a strong association between biallelic DLK1 expression and hypermethylation of a cytosine-phosphate-guanosine-rich region 18 kb upstream of DLK1. Allele-specific methylation analysis of this region revealed the alleles to be differentially methylated in normal bone marrow and monoallelic DLK1 AML, whereas there was increased methylation of both alleles in AML with biallelic expression. Moreover, chromatin immunoprecipitation analysis revealed that CCTC-binding factor binds to this region in monoallelic but not biallelic expression samples. Taken together, our data indicate that an insulator located 18 kb upstream of DLK1 plays an important role in regulating DLK1 imprinting.
机译:DLK1是第14号染色体上的印迹基因。使用信息编码的单核苷酸多态性,我们发现DLK1在正常骨髓中为单等位基因,而在过表达DLK1的76%的急性髓细胞白血病(AML)中它是双等位基因(占所有AML的61%) )。对7个富含胞嘧啶-磷酸-鸟苷的区域进行定量甲基化分析(DLK1上游或内部3个,推定的基因间差异甲基化区域以及MEG3上游或内部3个),发现等位基因DLK1表达与胞嘧啶-甲基化的高度甲基化之间有很强的联系在DLK1上游18 kb处富含磷酸-鸟苷的区域。该区域的等位基因特异性甲基化分析显示,等位基因在正常骨髓和单等位基因DLK1 AML中差异甲基化,而在具有双等位基因表达的AML中,这两个等位基因的甲基化增加。此外,染色质免疫沉淀分析表明,CCTC结合因子与单等位基因表达样品中的该区域结合,而与双等位基因表达样品中的该区域结合。综上所述,我们的数据表明位于DLK1上游18 kb的绝缘子在调节DLK1印迹中起重要作用。

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