N6-Methyladenosine: a conformational marker that regulates the substrate specificity of human demethylases FTO and ALKBH5

Zou, Shui; Toh, Joel D. W.; Wong, Kendra H. Q.; Gao, Yong‐Gui; Hong, Wanjin; Woon, Esther C. Y.

doi:10.1038/srep25677

Cited by 122 publications

(113 citation statements)

References 58 publications

(112 reference statements)

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“…The original studies on FTO-mediated m 6 A demethylation [25], as well as follow-up studies [46], showed that FTO efficiently demethylates m 6 A irrespective of sequence context. The original studies on FTO-mediated m 6 A demethylation [25], as well as follow-up studies [46], showed that FTO efficiently demethylates m 6 A irrespective of sequence context.…”

Section: Inconsistencies With M 6 a As The Substrate Of Ftomentioning

confidence: 99%

FTO, m⁶A_m, and the hypothesis of reversible epitranscriptomic mRNA modifications

Mauer

Jaffrey

2018

FEBS Letters

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The fate of mRNA is regulated by epitranscriptomic nucleotide modifications, the most abundant of which is N -methyladenosine (m A). Although the pattern and distribution of m A in mRNA is mediated by specific methyltransferases, a recent hypothesis is that specific demethylases or 'erasers' allow m A to be dynamically reversed by signaling pathways. In this Review, we discuss the data in support and against this model. New insights into the function of fat mass and obesity-associated protein (FTO), the original enzyme thought to be an m A eraser, reveal that its physiologic target is not m A, but instead is N ,2'-O-dimethyladenosine (m A ). Another m A demethylase, ALKBH5, appears to have functions limited to sperm development in normal mice. Overall, the majority of the data suggest that m A is generally not reversible, although m A may be susceptible to demethylation in pathophysiological states such as cancer.

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Section: Inconsistencies With M 6 a As The Substrate Of Ftomentioning

confidence: 99%

FTO, m⁶A_m, and the hypothesis of reversible epitranscriptomic mRNA modifications

Mauer

Jaffrey

2018

FEBS Letters

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“…The m6A demethylases: focus on FTO In mammals, two m6A demethylating enzymes have been identified to date, namely the fat mass and obesity-associated (FTO) protein (Jia et al 2011) and Alkbh5 (Zheng et al 2012). Both belong to the AlkB family of the Fe(II)/aketoglutarate-dependent dioxygenase superfamily and possess a similar catalytic core, although they have different substrate preferences (Aik et al 2014;Zou et al 2016) and are differentially expressed in different mammalian organs (Gerken et al 2007;Zheng et al 2012). ALKBH5 is highly expressed in testis and is essential for spermatogenesis (Zheng et al 2012).…”

Section: The M6a-machineriesmentioning

confidence: 99%

“…This not only indicates a compensatory mechanism driven by Alkbh5, but also raises the question of whether FTO and Alkbh5 have different substrate specificity. A modeling study of m6A containing RNAs suggests that the conformational change induced by m6A could be a critical factor for FTO or ALKBH5 recruitment (Zou et al 2016).…”

Section: The M6a-machineriesmentioning

confidence: 99%

The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

Widagdo

Anggono

2018

Journal of Neurochemistry

120

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Research over the past decade has provided strong support for the importance of various epigenetic mechanisms, including DNA and histone modifications in regulating activity-dependent gene expression in the mammalian central nervous system. More recently, the emerging field of epitranscriptomics revealed an equally important role of post-transcriptional RNA modifications in shaping the transcriptomic landscape of the brain. This review will focus on the methylation of the adenosine base at the N6 position, termed N methyladenosine (m6A), which is the most abundant internal modification that decorates eukaryotic messenger RNAs. Given its prevalence and dynamic regulation in the adult brain, the m6A-epitranscriptome provides an additional layer of regulation on RNA that can be controlled in a context- and stimulus-dependent manner. Conceptually, m6A serves as a molecular switch that regulates various aspects of RNA function, including splicing, stability, localization, or translational control. The versatility of m6A function is typically determined through interaction or disengagement with specific classes of m6A-interacting proteins. Here we review recent advances in the field and provide insights into the roles of m6A in regulating brain function, from development to synaptic plasticity, learning, and memory. We also discuss how aberrant m6A signaling may contribute to neurodevelopmental and neuropsychiatric disorders.

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“…15–17 Alkbh3 hydroxylates methyl lesions in single-stranded (ss) DNA as well as m 1 A in mRNA, thereby expanding the substrate range to RNA. 18 Alkbh5 and FTO also act on RNA, 19–22 but these enzymes demethylate 6-methyl adenine (m 6 A) in this substrate in vitro , affecting mRNA stability. 1 In vivo , Alkbh5 plays a role in fertility while FTO is important for controlling body weight in mice and humans.…”

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confidence: 99%

Biochemical Characterization of AP Lyase and m⁶A Demethylase Activities of Human AlkB Homologue 1 (ALKBH1)

et al. 2017

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Alkbh1 is one of nine mammalian homologs of Escherichia coli AlkB, a 2-oxoglutarate-dependent dioxygenase that catalyzes direct DNA repair by removing alkyl lesions from DNA. Six distinct enzymatic activities have been reported for Alkbh1, including hydroxylation of variously methylated DNA, mRNA, tRNA, or histone substrates along with the cleavage of DNA at apurinic/apyrimidinic (AP) sites followed by covalent attachment to the 5′-product. The studies described here extend the biochemical characterization for two of these enzymatic activities using human ALKBH1: the AP lyase and 6-methyl adenine DNA demethylase activities. The steady-state and single-turnover kinetic parameters for ALKBH1 cleavage of AP sites in DNA were determined and shown to be comparable to other AP lyases. The α,β-unsaturated aldehyde of the 5′-product arising from DNA cleavage reacts predominantly with C129 of ALKBH1, but secondary sites also generate covalent adducts. The 6-methyl adenine demethylase activity was examined with a newly developed assay using a methylation-sensitive restriction endonuclease, and the enzymatic rate was found to be very low. Indeed, the demethylase activity was less than half that of the AP lyase activity when ALKBH1 samples were assayed using identical buffer conditions. The two enzymatic activities were examined using a series of site-directed variant proteins, revealing the presence of distinct, but partially overlapping active sites for the two reactions. We postulate that the very low 6-methyl adenine oxygenase activity associated with ALKBH1 is unlikely to represent the major function of the enzyme in this cell, while the cellular role of the lyase activity (including its subsequent covalent attachment to DNA) remains uncertain.

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N6-Methyladenosine: a conformational marker that regulates the substrate specificity of human demethylases FTO and ALKBH5

Cited by 122 publications

References 58 publications

FTO, m⁶A_m, and the hypothesis of reversible epitranscriptomic mRNA modifications

FTO, m⁶A_m, and the hypothesis of reversible epitranscriptomic mRNA modifications

The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

Biochemical Characterization of AP Lyase and m⁶A Demethylase Activities of Human AlkB Homologue 1 (ALKBH1)

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N6-Methyladenosine: a conformational marker that regulates the substrate specificity of human demethylases FTO and ALKBH5

Cited by 122 publications

References 58 publications

FTO, m6Am, and the hypothesis of reversible epitranscriptomic mRNA modifications

FTO, m6Am, and the hypothesis of reversible epitranscriptomic mRNA modifications

The m6A‐epitranscriptomic signature in neurobiology: from neurodevelopment to brain plasticity

Biochemical Characterization of AP Lyase and m6A Demethylase Activities of Human AlkB Homologue 1 (ALKBH1)

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Product

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FTO, m⁶A_m, and the hypothesis of reversible epitranscriptomic mRNA modifications

FTO, m⁶A_m, and the hypothesis of reversible epitranscriptomic mRNA modifications

Biochemical Characterization of AP Lyase and m⁶A Demethylase Activities of Human AlkB Homologue 1 (ALKBH1)