Binding of actinomycin D to DNA: evidence for a nonclassical high-affinity binding mode that does not require GpC sites

  1. J G Snyder,
  2. N G Hartman,
  3. B L D'Estantoit,
  4. O Kennard,
  5. D P Remeta, and
  6. K J Breslauer
  1. University Chemical Laboratory, Cambridge, United Kingdom.

Abstract

We have employed a combination of temperature-dependent UV absorption spectroscopy, circular dichroism, and batch calorimetry to characterize the binding of actinomycin D to a series of oligomeric DNA duplexes. We find the duplex [d(CGTCGACG)]2 to be unique in its ability to bind actinomycin D strongly despite the absence of a classic GpC site. We present evidence that this non-GpC-containing duplex binds two actinomycin D molecules in an apparently cooperative manner to form a complex that exhibits aberrant spectroscopic and calorimetric behavior. We propose that these observations are consistent with actinomycin D exhibiting a high-affinity, sequence-dependent DNA-binding mode distinct from its classic binding to isolated GpC sites.

« Previous | Next Article »Table of Contents

This Article

  1. PNAS 1989-06 vol. 86 no. 11 3968-3972
  1. » Abstract
  2. Full Text (PDF)

Classifications

About Our New Site Design >>
Link: Advanced Search

This Week's Issue

  1. July 1, 2008, 105 (26)
  1. Current Issue
  1. Alert me to new issues of PNAS

Most