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Human and bacterial oxidative demethylases repair alkylation damage in both RNA and DNA

机译:人和细菌的氧化脱甲基酶可修复RNA和DNA中的烷基化损伤

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摘要

Repair of DNA damage is essential for maintaining genome integrity, and repair deficiencies in mammals are associated with cancer, neurological disease and developmental defects(1). Alkylation damage in DNA is repaired by at least three different mechanisms, including damage reversal by oxidative demethylation of 1-methyladenine and 3-methylcytosine by Escherichia coli AlkB(2,3). By contrast, little is known about consequences and cellular handling of alkylation damage to RNA(4). Here we show that two human AlkB homologues, hABH2 and hABH3, also are oxidative DNA demethylases and that AlkB and hABH3, but not hABH2, also repair RNA. Whereas AlkB and hABH3 prefer single-stranded nucleic acids, hABH2 acts more efficiently on double-stranded DNA. In addition, AlkB and hABH3 expressed in E. coli reactivate methylated RNA bacteriophage MS2 in vivo, illustrating the biological relevance of this repair activity and establishing RNA repair as a potentially important defence mechanism in living cells. The different catalytic properties and the different subnuclear localization patterns shown by the human homologues indicate that hABH2 and hABH3 have distinct roles in the cellular response to alkylation damage. [References: 27]
机译:DNA损伤的修复对于维持基因组完整性至关重要,而哺乳动物修复缺陷与癌症,神经系统疾病和发育缺陷有关(1)。至少可以通过三种不同的机制修复DNA中的烷基化损伤,包括通过大肠杆菌AlkB(2,3)对1-甲基腺嘌呤和3-甲基胞嘧啶进行氧化脱甲基化来逆转损伤。相比之下,人们对烷基化损害RNA的后果和细胞处理方法知之甚少(4)。在这里,我们显示了两个人类AlkB同源物hABH2和hABH3,也都是氧化性DNA脱甲基酶,而AlkB和hABH3(而非hABH2)也可以修复RNA。 AlkB和hABH3首选单链核酸,而hABH2对双链DNA的作用更高。此外,在大肠杆菌中表达的AlkB和hABH3可在体内重新激活甲基化的RNA噬菌体MS2,从而说明了这种修复活性的生物学相关性,并将RNA修复确立为活细胞中潜在的重要防御机制。人类同源物显示的不同的催化特性和不同的亚核定位模式表明,hABH2和hABH3在细胞对烷基化损伤的反应中具有不同的作用。 [参考:27]

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