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Role of the DNA methyltransferase variant DNMT3b3 in DNA methylation.

机译:DNA甲基转移酶变体DNMT3b3在DNA甲基化中的作用。

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Several alternatively spliced variants of DNA methyltransferase (DNMT) 3b have been described. Here, we identified new murine Dnmt3b mRNA isoforms and found that mouse embryonic stem (ES) cells expressed only Dnmt3b transcripts that contained exons 10 and 11, whereas the Dnmt3b transcripts in somatic cells lacked these exons, suggesting that this region is important for embryonic development. DNMT3b2 and 3b3 were the major isoforms expressed in human cell lines and the mRNA levels of these isoforms closely correlated with their protein levels. Although DNMT3b3 may be catalytically inactive, it still may be biologically important because D4Z4 and satellites 2 and 3 repeat sequences, all known DNMT3b target sequences, were methylated in cells that predominantly expressed DNMT3b3. Treatment of cells with the mechanism-based inhibitor 5-aza-2'-deoxycytidine (5-Aza-CdR) caused a complete depletion of DNMT1, 3a, 3b1, and 3b2 proteins. Human DNMT3b3 and the murine Dnmt3b3-like isoform, Dnmt3b6, were also depleted although less efficiently, suggesting that DNMT3b3 also may be capable of DNA binding. Moreover, de novo methylation of D4Z4 in T24 cancer cells after 5-Aza-CdR treatment only occurred when DNMT3b3 was expressed, reinforcing its role as a contributing factor of DNA methylation. The expression of either DNMT3b2 or 3b3, however, was not sufficient to explain the abnormal methylation of DNMT3b target sequences in human cancers, which may therefore be dependent on factors that affect DNMT3b targeting. Methylation analyses of immunodeficiency, chromosomal instabilities, and facial abnormalities cells revealed that an Alu repeat sequence was highly methylated, suggesting that Alu sequences are not DNMT3b targets.
机译:已描述了DNA甲基转移酶(DNMT)3b的几种可变剪接变体。在这里,我们发现了新的鼠Dnmt3b mRNA亚型,发现小鼠胚胎干(ES)细胞仅表达含有外显子10和11的Dnmt3b转录本,而体细胞中的Dnmt3b转录本却缺少这些外显子,这表明该区域对于胚胎发育很重要。 DNMT3b2和3b3是人类细胞系中表达的主要同工型,这些同工型的mRNA水平与其蛋白质水平密切相关。尽管DNMT3b3可能是无催化活性的,但由于D4Z4以及卫星2和3重复序列(所有已知的DNMT3b靶序列)在主要表达DNMT3b3的细胞中被甲基化,因此它在生物学上仍然很重要。用基于机理的抑制剂5-氮杂2'-脱氧胞苷(5-Aza-CdR)处理细胞会导致DNMT1、3a,3b1和3b2蛋白完全耗尽。人DNMT3b3和鼠Dnmt3b3样亚型Dnmt3b6也被消耗掉了,尽管效率较低,这表明DNMT3b3也可能具有DNA结合能力。此外,仅在表达DNMT3b3时,才发生5-Aza-CdR处理后T24癌细胞中D4Z4的从头甲基化,从而增强了其作为DNA甲基化的作用因子的作用。然而,DNMT3b2或3b3的表达不足以解释DNMT3b靶序列在人类癌症中的异常甲基化,因此可能取决于影响DNMT3b靶向的因素。免疫缺陷,染色体不稳定和面部异常细胞的甲基化分析显示,Alu重复序列高度甲基化,表明Alu序列不是DNMT3b靶标。

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