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Light-induced control of protein destruction by opto-PROTAC.

Jing LiuHe ChenLeina MaZhixiang HeDong WangYi LiuQian LinTinghu ZhangNathanael S GrayH Ümit KaniskanJian JinWenyi Wei
Published in: Science advances (2020)
By hijacking endogenous E3 ligase to degrade protein targets via the ubiquitin-proteasome system, PROTACs (PRoteolysis TArgeting Chimeras) provide a new strategy to inhibit protein targets that were regarded as undruggable before. However, the catalytic nature of PROTAC potentially leads to uncontrolled degradation that causes systemic toxicity issues, limiting the application of PROTAC in the clinic. Here, we introduce a light-inducible switch on PROTACs, thereafter termed as opto-PROTAC, to enable the degradation of protein targets in a spatiotemporal manner. By adding a photolabile caging group on pomalidomide as a parental compound and two additional PROTACs, dBET1 and dALK, we demonstrated light-inducible protein degradation. These opto-PROTACs display no activities in the dark, while the restricted degradation can be induced at a specific time and rate by ultraviolet A irradiation. Our approach provides a generalizable platform for the development of light-controlled PROTACs and enables PROTAC to be a precision medicine.
Keyphrases
  • protein protein
  • amino acid
  • primary care
  • oxidative stress
  • drug delivery
  • high glucose