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New Dibenzoquinoxalines Inhibit Triple-Negative Breast Cancer Growth by Dual Targeting of Topoisomerase 1 and the <i>c-MYC</i> G-Quadruplex

Ming-Hao Hu, Jia-Hong Lin

2021Journal of Medicinal Chemistry43 citationsDOI

Abstract

As c-MYC is one of the central players in triple-negative breast cancer (TNBC) oncogenesis, inhibiting c-MYC expression would be an effective anticancer strategy. Transcription-induced negative supercoiling is crucial in the regulation of c-MYC transcription, which facilitates the formation of a G4 structure in NHE III1 that can silence the transcription. However, topoisomerase 1 (Topo1) can dissipate this negative supercoiling, leading to continuous activation of c-MYC transcription. Thus, dual ligands targeting both Topo1 and c-MYC G4 appear to be significant in cancer therapy. In this study, a series of new dibenzoquinoxaline derivatives were designed, synthesized, and evaluated for both Topo1 and c-MYC inhibition. Among them, 5 was identified as the most promising dual ligand, which could effectively inhibit Topo1 activity and strongly stabilize c-MYC G4, thereby inhibiting cancer cell growth. Accordingly, this work suggests that this dual-targeting strategy may be effective in cancer therapy.

Topics & Concepts

ChemistryCancer researchTopoisomeraseTranscription (linguistics)G-quadruplexTranscription factorCarcinogenesisDNA supercoilCancer cellTriple-negative breast cancerCell growthBreast cancerCancerBiologyBiochemistryDNAGeneGeneticsLinguisticsPhilosophyDNA replicationCancer therapeutics and mechanismsDNA and Nucleic Acid ChemistryAdvanced biosensing and bioanalysis techniques
New Dibenzoquinoxalines Inhibit Triple-Negative Breast Cancer Growth by Dual Targeting of Topoisomerase 1 and the <i>c-MYC</i> G-Quadruplex | Litcius