Reversal of DNA alkylation damage by two human dioxygenases

Duncan, Tod; Trewick, Sarah C.; Koivisto, Pertti; Bates, Paul A.; Lindahl, Tomas; Sedgwick, Barbara

doi:10.1073/pnas.262589799

Cited by 368 publications

(392 citation statements)

References 29 publications

(32 reference statements)

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“…m 1 A has recently been discovered as another mRNA modification, in addition to m 6 A, pseudouridine, and m 5 C. The presence of m 1 A at the 5′ UTR region in mRNA has been suggested to promote translation (Dominissini et al, 2016;Li et al, 2016). ALKBH3, a DNA repair enzyme that demethylates N 1 -methyldeoxyadenosine in single-stranded DNA (Aas et al, 2003;Duncan et al, 2002) has been suggested as a potential demethylase of m 1 A in mRNA , the functional relevance of which still requires further investigations. ALKBH3 is also capable of repairing tRNA alkylation damages (Aas et al, 2003), again the biological relevance of which was not clear.…”

Section: Trna M 1 a Demethylation By Alkbh1mentioning

confidence: 99%

ALKBH1-Mediated tRNA Demethylation Regulates Translation

Liu¹,

Clark²,

Luo³

et al. 2016

Cell

146

190

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SummaryTransfer RNA (tRNA) is a central component of protein synthesis and cell signaling network. One salient feature of tRNA is its heavily modified status, which can critically impact its function. Here we show that mammalian ALKBH1 is a tRNA demethylase. It mediates the demethylation of N 1 -methyladenosine (m 1 A) in tRNAs. The ALKBH1-catalyzed demethylation of the target tRNAs results in attenuated translation initiation and their decreased usage in protein synthesis. This process is dynamic and responds to glucose availability to affect translation. Our results uncover reversible methylation of tRNA as a new regulatory mechanism of post-transcriptional gene expression. In briefReversible tRNA methylation helps translation respond to nutrient availability.

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Section: Trna M 1 a Demethylation By Alkbh1mentioning

confidence: 99%

ALKBH1-Mediated tRNA Demethylation Regulates Translation

Liu¹,

Clark²,

Luo³

et al. 2016

Cell

146

190

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“…AlkB repairs various modifications as shown by the survival of alkylated bacteriophage in an E. coli alkB mutant [32,37,46,60,61]. Mainly, AlkB is known for the repair of 1-meA and 3-meC.…”

Section: Substratesmentioning

confidence: 99%

“…3, and studies have confirmed that 1-ethyladenine is repaired by AlkB to form adenine [37]. The C-1 C-H group rather than the C-2 C-H group of the ethyl adduct is oxidized, forming acetaldehyde as the released product along with the repaired base [37].S N 2 alkylating epoxides can cause hydroxyalkylated DNA lesions. For instance, ethylene oxide and propylene oxide can form 1-hydroxyalkyladenine and 3-hydroxyalkylcytosine.…”

mentioning

confidence: 99%

Oxidative dealkylation DNA repair mediated by the mononuclear non-heme iron AlkB proteins

Mishina

2006

Journal of Inorganic Biochemistry

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DNA can be damaged by various intracellular and environmental alkylating agents to produce alkylation base lesions. These base damages, if not repaired promptly, may cause genetic changes that lead to diseases such as cancer. Recently, it was discovered that some of the alkylation DNA base damage can be directly removed by a family of proteins called the AlkB proteins that utilize a mononuclear non-heme iron(II) and α-ketoglutarate as cofactor and cosubstrate. These proteins activate dioxygen and perform an unprecedented oxidative deal-kylation of the alkyl adducts on DNA heteroatoms. This review summarizes the discovery of this activity and the recent research advances in studying this unique DNA repair pathway. The focus is placed on the chemical mechanism and function of these proteins. KeywordsDNA repair; AlkB; ABH; Direct repair; Mononuclear non-heme iron; Dioxygenase; Oxidative dealkylation; Demethylation Direct repair of alkylation DNA damageCellular DNA is subject to nonenzymatic alkylation (methylation) by environmental or chemical mutagens, resulting in adducts that are toxic and mutagenic [1][2][3][4][5][6]. Organisms have evolved a variety of mechanisms to repair these mutagenic damages. Escherichia coli (E. coli) responds to this threat by activating an adaptive responsive pathway, mediated by the E. coli Ada protein [7]. Upon receiving a methyl group from the damaged DNA, Ada turns into a transcriptional activator and activates its own expression and that of the alkB gene and two other genes, alkA and aidB ( Fig. 1(a)) [4,7,8]. The upregulated Ada is a bifunctional protein, which uses a N-terminal Cys38 residue to remove a methyl group fromS p -methylphosphotriester and a C-terminal Cys321 residue to remove a methyl adduct from O 6 -methylguanaine ( Fig. 1(b)) [9][10][11]. Both repair functions are irreversible and represent rare examples of direct repair of DNA damage. AlkA is a glycosylase that cleaves methylated bases from DNA and performs the first step of the well-known base excision repair of base lesions [12][13][14]. The precise function of AidB is still unknown. The function of the last member of this adaptive response, AlkB, also remained unknown until recently despite extensive research efforts. E. coli AlkBSince the first genetic study in 1983 isolating the E. coli mutant with specific sensitivity to the alkylating agent methylmethane sulfonate, MMS [15], the activity of AlkB was undisclosed The Fe II /αKG-dependent dioxygenase superfamily is widespread from bacteria to humans [19] and is the largest known non-heme iron protein family [20][21][22][23]. It represents a wide diversity of enzymes that catalyze the hydroxylation of unactivated C-H groups of a variety of substrates by coupling reductive activation of dioxygen with a decarbox-ylation of αKG, the co-substrate, to succinate. In the event of oxidation one of the oxygen atoms from O 2 is incorporated into the succinate and the other as a hydroxyl in the product [24]. This group of enzymes is known for their importance in ...

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“…AlkB, hABH1, hABH2 and hABH3 have a similar specificity for 1-meA and 3-meC, but they exibit different selectivity for ss or double-stranded (ds) DNA/RNA substrates. hABH2 was found to be strikingly more active on dsDNA than on ssDNA (Duncan et al, 2002;Aas et al, 2003). By contrast, hABH1 and hABH3 strongly prefer ssDNA/RNA as substrates (Duncan et al, 2002;Aas et al, 2003;Westbye et al, 2008), whereas AlkB has a slightly higher activity toward ss than ds nucleic acids (Falnes et al, 2002).…”

Section: Alkb-family Dna/rna Demethylase and Substrate Selection Mechmentioning

confidence: 93%

“…Eight AlkB homologs are predicted to exist in human (Kurowski et al, 2003). Removal of the methyl group from 1-methyladenine (1-meA) and 3-methylcytosine (3-meC) through oxidation by AlkB family protein has been experimentally demonstrated for E. coli AlkB (Falnes et al, 2002) and its human homologs hABH1 (Westbye et al, 2008;Müller et al, 2010), hABH2 (Duncan et al, 2002;Aas et al, 2003) and hABH3 (Duncan et al, 2002). In addition to DNA, RNA can also act as substrates of some AlkB members like AlkB, hABH1 and hABH3 (Aas et al, 2003;Westbye et al, 2008).…”

Section: Alkb-family Dna/rna Demethylase and Substrate Selection Mechmentioning

confidence: 99%

A loop matters for FTO substrate selection

et al. 2010

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Recent studies have unequivocally established the link between FTO and obesity. FTO was biochemically shown to belong to the AlkB-like family DNA/RNA demethylase. However, FTO differs from other AlkB members in that it has unique substrate specificity and contains an extended C-terminus with unknown functions. Insight into the substrate selection mechanism and a functional clue to the C-terminus of FTO were gained from recent structural and biochemical studies. These data would be valuable to design FTO-specific inhibitors that can be potentially translated into therapeutic agents for treatment of obesity or obesity-related diseases.

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Reversal of DNA alkylation damage by two human dioxygenases

Cited by 368 publications

References 29 publications

ALKBH1-Mediated tRNA Demethylation Regulates Translation

ALKBH1-Mediated tRNA Demethylation Regulates Translation

Oxidative dealkylation DNA repair mediated by the mononuclear non-heme iron AlkB proteins

A loop matters for FTO substrate selection

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