Structural basis for the recognition of diastereomeric 5′,8-cyclo-2′-deoxypurine lesions by the human nucleotide excision repair system

The hydroxyl radical is a powerful oxidant that generates DNA lesions including the stereoisomeric R and S 5′,8-cyclo-2′-deoxyadenosine (cdA) and 5′,8-cyclo-2′-deoxyguanosine (cdG) pairs that have been detected in cellular DNA. Unlike some other oxidatively generated DNA lesions, cdG and cdA are rep...

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Published inNucleic acids research Vol. 42; no. 8; pp. 5020 - 5032
Main Authors Kropachev, Konstantin, Ding, Shuang, Terzidis, Michael A., Masi, Annalisa, Liu, Zhi, Cai, Yuqin, Kolbanovskiy, Marina, Chatgilialoglu, Chryssostomos, Broyde, Suse, Geacintov, Nicholas E., Shafirovich, Vladimir
Format Journal Article
LanguageEnglish
Published England Oxford University Press 01.04.2014
Subjects
Deoxyadenosines - chemistry
Deoxyguanosine - analogs & derivatives
Deoxyguanosine - chemistry
DNA - chemistry
DNA Damage
DNA Repair
Genome Integrity, Repair and
HeLa Cells
Humans
Molecular Dynamics Simulation
Nucleic Acid Conformation
Stereoisomerism
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Summary:The hydroxyl radical is a powerful oxidant that generates DNA lesions including the stereoisomeric R and S 5′,8-cyclo-2′-deoxyadenosine (cdA) and 5′,8-cyclo-2′-deoxyguanosine (cdG) pairs that have been detected in cellular DNA. Unlike some other oxidatively generated DNA lesions, cdG and cdA are repaired by the human nucleotide excision repair (NER) apparatus. The relative NER efficiencies of all four cyclopurines were measured and compared in identical human HeLa cell extracts for the first time under identical conditions, using identical sequence contexts. The cdA and cdG lesions were excised with similar efficiencies, but the efficiencies for both 5′R cyclopurines were greater by a factor of ∼2 than for the 5′S lesions. Molecular modeling and dynamics simulations have revealed structural and energetic origins of this difference in NER-incision efficiencies. These lesions cause greater DNA backbone distortions and dynamics relative to unmodified DNA in 5′R than in 5′S stereoisomers, producing greater impairment in van der Waals stacking interaction energies in the 5′R cases. The locally impaired stacking interaction energies correlate with relative NER incision efficiencies, and explain these results on a structural basis in terms of differences in dynamic perturbations of the DNA backbone imposed by the R and S covalent 5′,8 bonds.
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ISSN:0305-1048
1362-4962
DOI:10.1093/nar/gku162