JOURNAL ARTICLE

Solution Structure of a 2:1 Quindoline–c-MYC G-Quadruplex: Insights into G-Quadruplex-Interactive Small Molecule Drug Design

Jixun DaiMegan CarverLaurence H. HurleyDanzhou Yang

Year: 2011 Journal:   Journal of the American Chemical Society Vol: 133 (44)Pages: 17673-17680   Publisher: American Chemical Society

Abstract

Unimolecular parallel-stranded G-quadruplex structures are found to be prevalent in gene promoters. The nuclease hypersensitivity element III(1) (NHE III(1)) of the c-MYC promoter can form transcriptionally active and silenced forms, and the formation of DNA G-quadruplex structures has been shown to be critical for c-MYC transcriptional silencing. The solution structure of a 2:1 quindoline-G-quadruplex complex has been solved and shows unexpected features, including the drug-induced reorientation of the flanking sequences to form a new binding pocket. While both 3' and 5' complexes show overall similar features, there are identifiable differences that emphasize the importance of both stacking and electronic interactions. For the first time, we describe the importance of the shape of the ligand as well as the two flanking bases in determining drug binding specificity. These structures provide important insights for the structure-based rational design of drugs that bind to unimolecular parallel G-quadruplexes commonly found in promoter elements.

Keywords:
G-quadruplex Chemistry Stacking Rational design Nuclease Small molecule DNA Promoter Drug design Gene silencing Stereochemistry Molecule Ligand (biochemistry) Anticancer drug Gene Computational biology Drug Biochemistry Genetics Gene expression Biology Pharmacology Receptor

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370
Cited By
7.13
FWCI (Field Weighted Citation Impact)
46
Refs
0.98
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Is in top 1%
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Citation History

Topics

DNA and Nucleic Acid Chemistry
Life Sciences →  Biochemistry, Genetics and Molecular Biology →  Molecular Biology
Advanced biosensing and bioanalysis techniques
Life Sciences →  Biochemistry, Genetics and Molecular Biology →  Molecular Biology
RNA Interference and Gene Delivery
Life Sciences →  Biochemistry, Genetics and Molecular Biology →  Molecular Biology

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