Interaction of a Cationic Porphyrin and Its Metal Derivatives with G‑Quadruplex DNA

Interaction of a Cationic Porphyrin and Its Metal Derivatives with G‑Quadruplex DNA

G-quadruplex (GQ) structures formed from guanine-rich sequences are found throughout the genome and are overrepresented in the promoter regions of some oncogenes, at the telomeric ends of eukaryotic chromosomes, and at the 5′-untranslated regions of mRNA. Interaction of small molecule ligands with G...

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Bibliographic Details
Published in:The journal of physical chemistry. B Vol. 120; no. 50; pp. 12807 - 12819
Main Authors: Boschi, Eric, Davis, Supriya, Taylor, Scott, Butterworth, Andrew, Chirayath, Lilyan A, Purohit, Vaishali, Siegel, Laura K, Buenaventura, Janesha, Sheriff, Alexandra H, Jin, Rowen, Sheardy, Richard, Yatsunyk, Liliya A, Azam, Mahrukh
Format: Journal Article
Language:English
Published: United States American Chemical Society 22-12-2016
Subjects:
5' Untranslated Regions
Binding Sites
Coordination Complexes - chemistry
Copper - chemistry
G-Quadruplexes
Guanine - chemistry
Metalloporphyrins - chemistry
Nucleic Acid Conformation
Porphyrins - chemistry
Potassium - chemistry
Sodium - chemistry
Solutions
Thermodynamics
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Summary:G-quadruplex (GQ) structures formed from guanine-rich sequences are found throughout the genome and are overrepresented in the promoter regions of some oncogenes, at the telomeric ends of eukaryotic chromosomes, and at the 5′-untranslated regions of mRNA. Interaction of small molecule ligands with GQ DNA is an area of great research interest to develop novel anticancer therapeutics and GQ sensors. In this paper we examine the interactions of TMPyP4, its isomer TMPyP2 (containing N-methyl-2-pyridyl substituents, N-Me-2Py) as well as two metal derivatives ZnTMPyP4 and CuTMPyP4 with GQs formed by dT4G4 and dT4G4T in 100 mM K+ or Na+ conditions. The DNA sequences were chosen to elucidate the effect of the 3′-T on the stabilization effect of porphyrins, binding modes, affinities, and stoichiometries determined via circular dichroism melting studies, UV–vis titrations, continuous variation analysis, and fluorescence studies. Our findings demonstrate that the stabilizing abilities of porphyrins are stronger toward (dT4G4)4 as compared to (dT4G4T)4 (ΔT m is 4.4 vs −6.4 for TMPyP4; 12.7 vs 5.7 for TMPyP2; 16.4 vs 12.1 for ZnTMPyP4; and 1.9 vs −8.4 °C for CuTMPyP4) suggesting that the 3′G-tetrad presents at least one of the binding sites. The binding affinity was determined to be moderate (K a ∼ 106–107 μM–1) with a typical binding stoichiometry of 1:1 or 2:1 porphyrin-to-GQ. In all studies, ZnTMPyP4 emerged as a ligand superior to TMPyP4. Overall, our work contributes to clearer understanding of interactions between porphyrins and GQ DNA.
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ISSN:1520-6106
1520-5207
DOI:10.1021/acs.jpcb.6b09827