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The human DNA methyltransferases (DNMTs) 1, 3a and 3b: coordinate mRNA expression in normal tissues and overexpression in tumors.

机译:人类DNA甲基转移酶(DNMT)1、3a和3b:协调正常组织中的mRNA表达和肿瘤中的过度表达。

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摘要

DNA methylation in mammals is required for embryonic development, X chromosome inactivation and imprinting. Previous studies have shown that methylation patterns become abnormal in malignant cells and may contribute to tumorigenesis by improper de novo methylation and silencing of the promoters for growth-regulatory genes. RNA and protein levels of the DNA methyltransferase DNMT1 have been shown to be elevated in tumors, however murine stem cells lacking Dnmt1 are still able to de novo methylate viral DNA. The recent cloning of a new family of DNA methyltransferases (Dnmt3a and Dnmt3b) in mouse which methylate hemimethylated and unmethylated templates with equal efficiencies make them candidates for the long sought de novo methyltransferases. We have investigated the expression of human DNMT1, 3a and 3b and found widespread, coordinate expression of all three transcripts in most normal tissues. Chromosomal mapping placed DNMT3a on chromosome 2p23 and DNMT3b on chromosome 20q11.2. Significant overexpression of DNMT3b was seen in tumors while DNMT1 and DNMT3a were only modestly over-expressed and with lower frequency. Lastly, several novel alternatively spliced forms of DNMT3b, which may have altered enzymatic activity, were found to be expressed in a tissue-specific manner.
机译:哺乳动物的DNA甲基化是胚胎发育,X染色体失活和印迹所必需的。先前的研究表明,甲基化模式在恶性细胞中变得异常,并可能通过不适当的从头甲基化和沉默生长调节基因的启动子而导致肿瘤发生。 DNA甲基转移酶DNMT1的RNA和蛋白质水平已显示在肿瘤中升高,但是缺乏Dnmt1的鼠干细胞仍然能够从头甲基化病毒DNA。最近在小鼠中克隆了一个新的DNA甲基转移酶新家族(Dnmt3a和Dnmt3b),它们以相同的效率甲基化半甲基化和未甲基化的模板,使它们成为长期寻求的从头甲基转移酶的候选者。我们已经研究了人DNMT1、3a和3b的表达,并发现在大多数正常组织中所有三个转录本的广泛协调表达。染色体作图法将DNMT3a置于2p23号染色体上,并将DNMT3b置于20q11.2号染色体上。 DNMT3b在肿瘤中显着过表达,而DNMT1和DNMT3a仅适度过表达且发生率较低。最后,发现可能具有改变的酶促活性的DNMT3b的几种新的可变剪接形式以组织特异性方式表达。

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