posted on 2022-02-15, 05:35authored bySilong Zhang, Yuanyuan Li, Tao Li, Yu Zhang, Haimei Li, Zhengzai Cheng, Na Peng, Yi Liu, Juan Xu, Huan He
Targeted
protein degradation technologies (e.g., PROTACs)
that can selectively degrade intracellular protein are
an emerging class of promising therapeutic modalities. Herein, we
describe the conjugation of photosensitizers and protein ligands (PS-Degrons),
as an activable targeted protein degradation platform. PS-Degrons
are capable of degrading protein of interest via light-triggered 1O2, which is orthogonal and complementary to existing
technologies. This generalizable platform allows controllable knockdown
of the target protein with high spatiotemporal precision. Our lead
compound PSDalpha induces a complete degradation of human estrogen
receptor α (ERα) under visible light. The high degrading
ERα efficacy of PSDalpha enables an excellent anti-proliferation
performance on MCF-7 cells. Our results establish a modular strategy
for the controllable degradation of target proteins, which can hopefully
overcome the systemic toxicity in clinical treatment of PROTACs. We
anticipate that PS-Degrons would open a new chapter for biochemical
research and for the therapeutics.