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N 6 -Methyladenine DNA Modification in the Human Genome

DNA N -methyladenine (6mA) modification is the most prevalent DNA modification in prokaryotes, but whether it exists in human cells and whether it plays a role in human diseases remain enigmatic. Here, we showed that 6mA is extensively present in the human genome, and we cataloged 881,240 6mA sites...

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Published in:Molecular cell 2018-07, Vol.71 (2), p.306
Main Authors: Xiao, Chuan-Le, Zhu, Song, He, Minghui, Chen, De, Zhang, Qian, Chen, Ying, Yu, Guoliang, Liu, Jinbao, Xie, Shang-Qian, Luo, Feng, Liang, Zhe, Wang, De-Peng, Bo, Xiao-Chen, Gu, Xiao-Feng, Wang, Kai, Yan, Guang-Rong
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container_title Molecular cell
container_volume 71
creator Xiao, Chuan-Le
Zhu, Song
He, Minghui
Chen, De
Zhang, Qian
Chen, Ying
Yu, Guoliang
Liu, Jinbao
Xie, Shang-Qian
Luo, Feng
Liang, Zhe
Wang, De-Peng
Bo, Xiao-Chen
Gu, Xiao-Feng
Wang, Kai
Yan, Guang-Rong
description DNA N -methyladenine (6mA) modification is the most prevalent DNA modification in prokaryotes, but whether it exists in human cells and whether it plays a role in human diseases remain enigmatic. Here, we showed that 6mA is extensively present in the human genome, and we cataloged 881,240 6mA sites accounting for ∼0.051% of the total adenines. [G/C]AGG[C/T] was the most significantly associated motif with 6mA modification. 6mA sites were enriched in the coding regions and mark actively transcribed genes in human cells. DNA 6mA and N -demethyladenine modification in the human genome were mediated by methyltransferase N6AMT1 and demethylase ALKBH1, respectively. The abundance of 6mA was significantly lower in cancers, accompanied by decreased N6AMT1 and increased ALKBH1 levels, and downregulation of 6mA modification levels promoted tumorigenesis. Collectively, our results demonstrate that DNA 6mA modification is extensively present in human cells and the decrease of genomic DNA 6mA promotes human tumorigenesis.
doi_str_mv 10.1016/j.molcel.2018.06.015
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