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Structural Modification of Noscapine via Photoredox/Nickel Dual Catalysis for the Discovery of S-Phase Arresting Agents.

Defeng LiChuanxu LiuTingyu GuoJiajie ZhuJiaqi GuoTing LuoYuhuan LiuWenhao ShenBiao JiangWei WangQianqian YinYongqiang Zhang
Published in: ACS medicinal chemistry letters (2024)
Herein, we disclose a powerful strategy for the functionalization of the antitumor natural alkaloid noscapine by utilizing photoredox/nickel dual-catalytic coupling technology. A small collection of 37 new noscapinoids with diverse (hetero)alkyl and (hetero)cycloalkyl groups and enhanced sp 3 character was thus synthesized. Further in vitro antiproliferative activity screening and SAR study enabled the identification of 6o as a novel, potent, and less-toxic anticancer agent. Furthermore, 6o exerts superior cellular activity via an unexpected S-phase arrest mechanism and could significantly induce cell apoptosis in a dose-dependent manner, thereby further highlighting its potential in drug discovery as a promising lead compound.
Keyphrases
  • drug discovery
  • visible light
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  • small molecule
  • reduced graphene oxide
  • high throughput
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  • cell cycle