Sequence-specific binding of luzopeptin to DNA | Zendy

Keith R. Fox | Zendy; Heather A. Davies | Zendy; Gill R. Adams | Zendy; José Portugal | Zendy; Michael J. Waring | Zendy

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Sequence-specific binding of luzopeptin to DNA

Author(s) -

Keith R. Fox,

Heather A. Davies,

Gill R. Adams,

José Portugal,

Michael J. Waring

Publication year - 1988

Publication title -

nucleic acids research

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 9.008

H-Index - 537

eISSN - 1362-4954

pISSN - 0305-1048

DOI - 10.1093/nar/16.6.2489

Subject(s) - biology , footprinting , dna , micrococcal nuclease , nuclease , dna footprinting , binding site , base pair , deoxyribonuclease i , biochemistry , dna binding protein , base sequence , gene , nucleosome , transcription factor , histone

We have examined the binding of luzopeptin, an antitumor antibiotic, to five DNA fragments of varying base composition. The drug forms a tight, possibly covalent, complex with the DNA causing a reduction in mobility on nondenaturing polyacrylamide gels and some smearing of the bands consistent with intramolecular cross-linking of DNA duplexes. DNAase I and micrococcal nuclease footprinting experiments suggest that the drug binds best to regions containing alternating A and T residues, although no consensus di- or trinucleotide sequence emerges. Binding to other sites is not excluded and at moderate ligand concentrations the DNA is almost totally protected from enzyme attack. Ligand-induced enhancement of DNAase I cleavage is observed at both AT and GC-rich regions. The sequence selectivity and characteristics of luzopeptin binding are quite different from those of echinomycin, a bifunctional intercalator of related structure.

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