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Structural motifs and intramolecular interactions in non-canonical G-quadruplexes

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RSC CHEMICAL BIOLOGY
卷 2, 期 2, 页码 338-353

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ROYAL SOC CHEMISTRY
DOI: 10.1039/d0cb00211a

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  1. Deutsche Forschungsgemeinschaft [WE 1933/15-1]

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This article discusses the formation of G-quadruplex structures by guanine-rich DNA or RNA sequences in the presence of monovalent cations, and the methods used to identify nucleic acid segments prone to quadruplex formation. Depending on sequence context, these sequences may fold into various types of quadruplex structures.
Guanine(G)-rich DNA or RNA sequences can assemble or intramolecularly fold into G-quadruplexes formed through the stacking of planar G center dot G center dot G center dot G tetrads in the presence of monovalent cations. These secondary nucleic acid structures have convincingly been shown to also exist within a cellular environment exerting important regulatory functions in physiological processes. For identifying nucleic acid segments prone to quadruplex formation, a putative quadruplex sequence motif encompassing closely spaced tracts of three or more guanosines is frequently employed for bioinformatic search algorithms. Depending on the number and type of intervening residues as well as on solution conditions, such sequences may fold into various canonical G4 topologies with continuous G-columns. On the other hand, a growing number of sequences capable of quadruplex formation feature G-deficient guanine tracts, escaping the conservative consensus motif. By folding into non-canonical quadruplex structures, they adopt unique topologies depending on their specific sequence context. These include G-columns with only two guanines, bulges, snapback loops, D- and V-shaped loops as well as interlocked structures. This review focuses on G-quadruplex species carrying such distinct structural motifs. It evaluates characteristic features of their non-conventional scaffold and highlights principles of stabilizing interactions that also allow for their folding into stable G-quadruplex structures.

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