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Reference - PMID:23245849 - Sculpting of DNA at abasic sites by DNA glycosylase homolog mag2.

Reference summary

PubMed ID
PMID:23245849
Title
Sculpting of DNA at abasic sites by DNA glycosylase homolog mag2.
Authors
Dalhus B, Nilsen L, Korvald H, Huffman J, Forstrøm RJ, McMurray CT, Alseth I, Tainer JA, Bjørås M
Citation
Structure 2013 Jan 08;21(1):154-166
Publication year
2013
Abstract
Modifications and loss of bases are frequent types of DNA lesions, often handled by the base excision repair (BER) pathway. BER is initiated by DNA glycosylases, generating abasic (AP) sites that are subsequently cleaved by AP endonucleases, which further pass on nicked DNA to downstream DNA polymerases and ligases. The coordinated handover of cytotoxic intermediates between different BER enzymes is most likely facilitated by the DNA conformation. Here, we present the atomic structure of Schizosaccharomyces pombe Mag2 in complex with DNA to reveal an unexpected structural basis for nonenzymatic AP site recognition with an unflipped AP site. Two surface-exposed loops intercalate and widen the DNA minor groove to generate a DNA conformation previously only found in the mismatch repair MutS-DNA complex. Consequently, the molecular role of Mag2 appears to be AP site recognition and protection, while possibly facilitating damage signaling by structurally sculpting the DNA substrate.

Annotation

GO biological process

GO:0006284 - base-excision repair

Genes:

GO:0006307 - DNA alkylation repair

Genes:

GO:0006289 - nucleotide-excision repair

Genes:

GO:0000725 - recombinational repair

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GO cellular component

GO:0005634 - nucleus

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GO molecular function

GO:0140431 - DNA-(abasic site) binding

Genes:

GO:0003905 - alkylbase DNA N-glycosylase activity

Genes:

Multi-locus phenotype

FYPO:0000089 - sensitive to methyl methanesulfonate

Genes:

Genotypes:

Single locus phenotype

FYPO:0000957 - normal growth on methyl methanesulfonate

Genes:

Genotypes:

FYPO:0000089 - sensitive to methyl methanesulfonate

Genes:

Genotypes: