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Structural studies on acridine derivatives binding to telomeric DNA

✍ Scribed by Shirley Miles; Philip Callow; Susana Teixeira; Yu Gan; William Denny; Chris Cardin; Trevor Forsyth


Book ID
103886489
Publisher
Elsevier Science
Year
2006
Tongue
English
Weight
152 KB
Volume
385-386
Category
Article
ISSN
0921-4526

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✦ Synopsis


Acridine derivatives can inhibit a variety of nuclear enzymes by binding or intercalating to DNA. This class of compounds is of great interest in the development of novel anticancer agents. Despite the availability of crystallographic data for some of the compounds complexed with DNA, uncertainties remain about the mechanisms of action, binding preferences and biological targets. To investigate the intercalation of several acridine derivatives, a variety of techniques are being employed. Single-crystal X-ray diffraction is being used to determine the high resolution three-dimensional structure of short sequences of quadruplex telomeric DNA with bound drug. This will be compared to the effect of drug binding to long segments of double-stranded DNA using fibre diffraction, with neutron diffraction studies planned to analyse the hydrogen bonding patterns of the DNA-drug complexes. Small-angle neutron scattering (SANS) will also be applied to study drug binding to both short and long sequences of quadruplex and double-stranded DNA in solution. Initial SANS measurements of the telomeric repeat d(TGGGGT) imply that this hexamer is present as a quadruplex.


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✍ D. J. Bleaks; S. S. Danyluk πŸ“‚ Article πŸ“… 1967 πŸ› Wiley (John Wiley & Sons) 🌐 English βš– 839 KB

## Synopsis Nuclear magnetic resoiiaiice spectra of acridine have been measured in aqueous methanol solutions over a wide concentration range in the presence and absence of dissolved UNA. In solutions containing DNA the acridiiie spectra show a marked line broadening and intensity decrease at temp