Litcius/Paper detail

Facilitated Drug Repurposing with Artemisinin-Derived PROTACs: Unveiling PCLAF as a Therapeutic Target

Yan Li, Zi Wei Zeng, Di Chen, Zhi Cheng Gu, Wan Li Yan, Ling Yun Yue, Ren Guang Zhu, Yong Zhao, Lei Chen, Qing Zhao, Bin He

2023Journal of Medicinal Chemistry31 citationsDOIOpen Access PDF

Abstract

Artemisinin, a prominent anti-malaria drug, is being investigated for its potential as a repurposed cancer treatment. However, its effectiveness in tumor cell lines remains limited, and its mechanism of action is unclear. To make more progress, the PROteolysis-TArgeting chimera (PROTAC) technique has been applied to design and synthesize novel artemisinin derivatives in this study. Among them, AD4, the most potent compound, exhibited an IC 50 value of 50.6 nM in RS4;11 cells, over 12-fold better than that of its parent compound, SM1044 . This was supported by prolonged survival of RS4;11-transplanted NOD/SCID mice. Meanwhile, AD4 effectively degraded PCLAF in RS4;11 cells and thus activated the p21/Rb axis to exert antitumor activity by directly targeting PCLAF. The discovery of AD4 highlights the great potential of using PROTACs to improve the efficacy of natural products, identify therapeutic targets, and facilitate drug repurposing. This opens a promising avenue for transforming other natural products into effective therapies.

Topics & Concepts

ArtemisininDrug repositioningChemistryDrugPharmacologyDrug targetRepurposingDrug discoveryMedicineMalariaBiochemistryPlasmodium falciparumImmunologyBiologyEcologyProtein Degradation and InhibitorsMultiple Myeloma Research and TreatmentsUbiquitin and proteasome pathways