Interstrand DNA Cross-Links Derived from Reaction of a 2-Aminopurine Residue with an Abasic Site.
Maryam Imani NejadNathan E PriceTuhin HaldarCalvin LewisYinsheng WangKent S GatesPublished in: ACS chemical biology (2019)
Efficient methods for the site-specific installation of structurally defined interstrand cross-links in duplex DNA may be useful in a wide variety of fields. The work described here developed a high-yield synthesis of chemically stable interstrand cross-links resulting from a reductive amination reaction between an abasic site and the noncanonical nucleobase 2-aminopurine in duplex DNA. Results from footprinting, liquid chromatography-mass spectrometry, and stability studies support the formation of an N2-alkylamine attachment between the 2-aminopurine residue and the Ap site. The reaction performs best when the 2-aminopurine residue on the opposing strand is offset 1 nt to the 5'-side of the abasic site. The cross-link confers substantial resistance to thermal denaturation (melting). The cross-linking reaction is fast (complete in 4 h), employs only commercially available reagents, and can be used to generate cross-linked duplexes in sufficient quantities for biophysical, structural, and DNA repair studies.
Keyphrases
- dna repair
- mass spectrometry
- liquid chromatography
- circulating tumor
- cell free
- single molecule
- high resolution
- dna damage
- high resolution mass spectrometry
- nucleic acid
- electron transfer
- case control
- high performance liquid chromatography
- amino acid
- simultaneous determination
- dna damage response
- tandem mass spectrometry
- circulating tumor cells
- solid phase extraction