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Design, synthesis, and DNA sequence selectivity of formaldehyde-mediated DNA-adducts of the novel N-(4-aminobutyl) acridine-4-carboxamide
journal contribution
posted on 2014-12-15, 00:00 authored by Elizabeth AnkersElizabeth Ankers, B J Evison, D R Phillips, R T C Brownlee, S M CuttsA novel derivative of the anti-tumor agent N-[2-(dimethylamino)ethyl]acridine-4-carboxamide (DACA) was prepared by reduction of 9-oxoacridan-4-carboxylic acid to acridine-4-carboxylic acid with subsequent conversion to N-(4-aminobutyl)acridine-4-carboxamide (C4-DACA). Molecular modeling studies suggested that a DACA analogue comprising a side chain length of four carbons was optimal to form formaldehyde-mediated drug-DNA adducts via the minor groove. An in vitro transcription assay revealed that formaldehyde-mediated C4-DACA-DNA adducts selectively formed at CpG and CpA dinucleotide sequences, which is strikingly similar to that of formaldehyde-activated anthracenediones such as pixantrone.
History
Journal
Bioorganic and medicinal chemistry lettersVolume
24Issue
24Pagination
5710 - 5715Publisher
ElsevierLocation
Amsterdam, The NetherlandsPublisher DOI
ISSN
0960-894XeISSN
1464-3405Language
engPublication classification
C Journal article; C1.1 Refereed article in a scholarly journalCopyright notice
2014, ElsevierUsage metrics
Keywords
Acridine-4-carboxamideDNA adductsEnergy minimized 3D modelFormaldehyde activationTranscription assayAcridinesCpG IslandsDisinfectantsDrug DesignFormaldehydeIsoquinolinesModels, MolecularMolecular StructureTopoisomerase II InhibitorsScience & TechnologyLife Sciences & BiomedicinePhysical SciencesChemistry, MedicinalChemistry, OrganicPharmacology & PharmacyChemistryINTERSTRAND CROSS-LINKSAZA-ANTHRACENEDIONEMASS-SPECTROMETRYCRYSTAL-STRUCTUREANTITUMOR AGENTSBREAST-CANCERADRIAMYCINMITOXANTRONEPIXANTRONEDAUNORUBICINOrganic Chemistry