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Second Generation G-Quadruplex Stabilizing Trimethine Cyanines.

Eric A OwensHang T HuynhEkaterina M StroevaArghya BarmanKostiantyn ZiabrevAnanya PaulSarah V NguyenMatthew LaramieDonald HamelbergMarkus W GermannW David WilsonMaged Henary
Published in: Bioconjugate chemistry (2019)
G-Quadruplex DNA has been recognized as a highly appealing target for the development of new selective chemotherapeutics, which could result in markedly reduced toxicity toward normal cells. In particular, the cyanine dyes that bind selectively to G-quadruplex structures without targeting duplex DNA have attracted attention due to their high amenability to structural modifications that allows fine-tuning of their biomolecular interactions. We have previously reported pentamethine and symmetric trimethine cyanines designed to effectively bind G-quadruplexes through end stacking interactions. Herein, we are reporting a second generation of drug candidates, the asymmetric trimethine cyanines. These have been synthesized and evaluated for their quadruplex binding properties. Incorporating a benz[c,d]indolenine heterocyclic unit increased overall quadruplex binding, and elongating the alkyl length increases the quadruplex-to-duplex binding specificity.
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