Interactions of small molecules with DNA junctions

Author:

McQuaid Kane T1,Pipier Angélique2,Cardin Christine J1,Monchaud David2ORCID

Affiliation:

1. Department of Chemistry, University of Reading , Whiteknights, Reading  RG6 6AD, UK

2. Institut de Chimie Moléculaire de l’Université de Bourgogne (ICMUB) , CNRS UMR 6302, UBFC Dijon, 21078 Dijon , France

Abstract

Abstract The four natural DNA bases (A, T, G and C) associate in base pairs (A=T and G≡C), allowing the attached DNA strands to assemble into the canonical double helix of DNA (or duplex-DNA, also known as B-DNA). The intrinsic supramolecular properties of nucleobases make other associations possible (such as base triplets or quartets), which thus translates into a diversity of DNA structures beyond B-DNA. To date, the alphabet of DNA structures is ripe with approximately 20 letters (from A- to Z-DNA); however, only a few of them are being considered as key players in cell biology and, by extension, valuable targets for chemical biology intervention. In the present review, we summarise what is known about alternative DNA structures (what are they? When, where and how do they fold?) and proceed to discuss further about those considered nowadays as valuable therapeutic targets. We discuss in more detail the molecular tools (ligands) that have been recently developed to target these structures, particularly the three- and four-way DNA junctions, in order to intervene in the biological processes where they are involved. This new and stimulating chemical biology playground allows for devising innovative strategies to fight against genetic diseases.

Funder

Agence Nationale de la Recherche

European Regional Development Fund

ISITE BFC

Publisher

Oxford University Press (OUP)

Subject

Genetics

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