Interaction of a macrocyclic bisacridine with DNA
- 1 December 1990
- journal article
- research article
- Published by American Chemical Society (ACS) in Biochemistry
- Vol. 29 (49) , 10918-10927
- https://doi.org/10.1021/bi00501a009
Abstract
The binding of the macrocycle SDM to DNA was investigated by visible spectroscopy, stopped-flow kinetics, and NMR spectroscopy. SDM is composed of two 9-aminoacridines linked via the amino groups by a spermine side chain and via the 4-positions by a N,N''-[(methylthio)ethyl]succinamide side chain [Zimmerman, S.C., Lamberson, C.R., Cory, M., and Fairley, T.A. (1989) J. Am. Chem. Soc. 111, 6805-6809]. The visible spectrum of SDM bound to poly[d(A-T)]2 or poly[d(G-C)]2 is red-shifted relative to the spectrum of SDM alone and displays considerable hypochromicity. Results from titrations of SDM with polymer indicate a binding site size of three base pairs per macrocycle. The dissociation constant for SDM bound to either poly[d(A-T)]2 or poly[d(G-C)]2 is an order of magnitude lower than that for a similar bisacridine linked only by a spermine side chain. In addition, the dependence of the dissociation constant on ionic strength is significantly reduced. NMR studies of SDM complexes with poly[d(A-T)]2 or a tetramer, d(CGCG)2, show that intercalation is the mode of binding. The magnitudes of the chemical shift differences for SDM aromatic protons in the free and bound states support intercalation with the acridine ring systems essentially parallel to the long axis of the base pairs. Cross peaks from NOESY spectra of the SDM complex with d(CGCG)2 further support this mode of binding and provide information on the structure of the complex. The results are analyzed for consistency with each of three binding models; (i) bisintercalation with the two side chains in the same groove; (ii) bisintercalation according to the neighbor-exclusion principle with the two side chains in opposite grooves; and (iii) bisintercalation with two side chains in opposite grooves but with violation of the neighbor-exclusion principle. Model i is found to be unlikely on the basis of all evidence obtained, including preliminary modeling studies. Both models ii and iii can be reconciled with the experimental evidence and from a modeling standpoint are energetically feasible.This publication has 24 references indexed in Scilit:
- Potential antitumor agents. 44. Synthesis and antitumor activity of new classes of diacridines: importance of linker chain rigidity for DNA binding kinetics and biological activityJournal of Medicinal Chemistry, 1985
- Mechanism of intercalation: Ion effects on the equilibrium and kinetic constants for the interaction of propidium and ethidium with DNABiopolymers, 1985
- Kinetics of dissociation of nogalamycin from DNA: comparison with other anthracycline antibioticsBiochimica et Biophysica Acta (BBA) - General Subjects, 1985
- Proton NMR study of the binding of bis(acridines) to d(AT)5.cntdot.d(AT)5. 1. Mode of bindingBiochemistry, 1985
- Polyelectrolyte effects on site‐binding equilibria with application to the intercalation of drugs into DNABiopolymers, 1984
- 1H‐ and 31P‐nuclear magnetic resonance studies on the conformation of d‐(CpGpCpG)2 and d‐(CpGpCpGpCpG)2 short helices in B‐conformationBiopolymers, 1984
- Effects of ring substituents and linker chains on the bifunctional intercalation of diacridines into deoxyribonucleic acidBiochemistry, 1980
- Structural limitations on the bifunctional intercalation of diacridines into DNABiochemistry, 1978
- Calculation of binding isotherms for heterogeneous polymersBiopolymers, 1968
- Studies of the binding of actinomycin and related compounds to DNAJournal of Molecular Biology, 1968