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Cytosine analogues as DNA methyltransferase substrates

Abstract:
DNA methyltransferases are drug targets for myelodysplastic syndrome (MDS), chronic myelomonocytic leukemia (CMML), acute myelogenous leukemia (AML) and possibly β-hemoglobinopathies. We characterize the interaction of nucleoside analogues in DNA with a prokaryotic CpG-specific DNA methyltransferase (M.MpeI) as a model for mammalian DNMT1 methyltransferases. We tested DNA containing 5-hydroxymethylcytosine (5hmC), 5-hydroxycytosine (5OHC), 5-methyl-2-pyrimidinone (in the ribosylated form known as 5-methylzebularine, 5mZ), 5,6-dihydro-5-azacytosine (dhaC), 5-fluorocytosine (5FC), 5-chlorocytosine (5ClC), 5-bromocytosine (5BrC) and 5-iodocytosine (5IC). Covalent complex formation was by far most efficient for 5FC. Non-covalent complexes were most abundant for dhaC and 5mZ. Surprisingly, we observed methylation of 5IC and 5BrC, and to a lesser extent 5ClC and 5FC, in the presence, but not the absence of small molecule thiol nucleophiles. For 5IC and 5BrC, we demonstrated by mass spectrometry that the reactions were due to methyltransferase driven dehalogenation, followed by methylation. Crystal structures of M.MpeI-DNA complexes capture the ‘in’ conformation of the active site loop for analogues with small or rotatable (5mZ) 5-substituents and its ‘out’ form for bulky 5-substituents. Since very similar ‘in’ and ‘out’ loop conformations were also observed for DNMT1, it is likely that our conclusions generalize to other DNA methyltransferases.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1093/nar/gkae568

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Author
ORCID:
0000-0002-8935-3640
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Author
ORCID:
0000-0002-5163-2855
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Institution:
University of Oxford
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Author
ORCID:
0000-0001-7942-2756
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Role:
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ORCID:
0000-0002-3449-7460
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Role:
Author
ORCID:
0000-0001-7884-4463


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Funder identifier:
https://ror.org/05pwfyy15
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Funder identifier:
https://ror.org/02jf81j23
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Funder identifier:
https://ror.org/048zd9m77


Publisher:
Oxford University Press
Journal:
Nucleic Acids Research More from this journal
Volume:
52
Issue:
15
Pages:
9267-9281
Publication date:
2024-07-05
Acceptance date:
2024-06-20
DOI:
EISSN:
1362-4962
ISSN:
0305-1048


Language:
English
Source identifiers:
2216253
Deposit date:
2024-08-27
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