Carrier-Free Nano-PROTACs to Amplify Photodynamic Therapy Induced DNA Damage through BRD4 Degradation.
Lin-Ping ZhaoXiao-Na RaoRong-Rong ZhengChu-Yu HuangRen-Jiang KongHong ChengBin LiShi-Ying LiPublished in: Nano letters (2023)
Therapy-induced DNA damage is the most common strategy to inhibit tumor cell proliferation, but the therapeutic efficacy is limited by DNA repair machinery. Carrier-free nanoproteolysis targeting chimeras (PROTACs), designed as SDNpros, have been developed to enhance photodynamic therapy (PDT) by blocking the DNA damage repair pathway through BRD4 degradation. Specifically, SDNpros are constructed through noncovalent interactions between the photosensitizer of chlorine e6 (Ce6) and PROTACs of BRD4 degrader (dBET57) via self-assembly. SDNpro has favorable dispersibility and a uniform nanosize distribution without drug excipients. Upon light irradiation, SDNpro produces abundant reactive oxygen species (ROS) to induce DNA oxidative damage. Meanwhile, the DNA repair pathway would be interrupted by the concurrent degradation of BRD4, which could intensify the oxidative DNA damage and elevate PDT efficiency. Beneficially, SDNpro suppresses tumor growth and avoids systemic side effects, providing a promising strategy to promote the clinical translation of PROTACs for tumor treatment.
Keyphrases
- dna damage
- photodynamic therapy
- dna repair
- fluorescence imaging
- oxidative stress
- reactive oxygen species
- diabetic rats
- dna damage response
- cell proliferation
- high glucose
- drug induced
- signaling pathway
- stem cells
- drinking water
- endothelial cells
- adverse drug
- circulating tumor
- combination therapy
- drug delivery
- bone marrow
- cell death
- mesenchymal stem cells
- cell therapy