Indoloquinoline-Mediated Targeted Downregulation of KRAS through Selective Stabilization of the Mid-Promoter G-Quadruplex Structure

KRAS is a well-validated anti-cancer therapeutic target, whose transcriptional downregulation has been demonstrated to be lethal to tumor cells with aberrant KRAS signaling. G-quadruplexes (G4s) are non-canonical nucleic acid structures that mediate central dogmatic events, such as DNA repair, telom...

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Bibliographic Details
Main Authors: Alexandra Maria Psaras, Rhianna K. Carty, Jared T. Miller, L. Nathan Tumey, Tracy A. Brooks
Format: Article
Language:English
Published: MDPI AG 2022-08-01
Series:Genes
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Online Access:https://www.mdpi.com/2073-4425/13/8/1440
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Summary:KRAS is a well-validated anti-cancer therapeutic target, whose transcriptional downregulation has been demonstrated to be lethal to tumor cells with aberrant KRAS signaling. G-quadruplexes (G4s) are non-canonical nucleic acid structures that mediate central dogmatic events, such as DNA repair, telomere elongation, transcription and splicing events. G4s are attractive drug targets, as they are more globular than B-DNA, enabling more selective gene interactions. Moreover, their genomic prevalence is increased in oncogenic promoters, their formation is increased in human cancers, and they can be modulated with small molecules or targeted nucleic acids. The putative formation of multiple G4s has been described in the literature, but compounds with selectivity among these structures have not yet been able to distinguish between the biological contribution of the predominant structures. Using cell free screening techniques, synthesis of novel indoloquinoline compounds and cellular models of KRAS-dependent cancer cells, we describe compounds that choose between KRAS promoter G4<sub>near</sub> and G4<sub>mid</sub>, correlate compound cytotoxic activity with KRAS regulation, and highlight G4<sub>mid</sub> as the lead molecular non-canonical structure for further targeting efforts.
ISSN:2073-4425