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Photoactivatable Prodrug-Backboned Polymeric Nanoparticles for Efficient Light-Controlled Gene Delivery and Synergistic Treatment of Platinum-Resistant Ovarian Cancer
124
Citations
48
References
2020
Year
Combination of chemotherapy and gene therapy provides an effective strategy for cancer treatment. However, the lack of suitable codelivery systems with efficient endo/lysosomal escape and controllable drug release/gene unpacking is the major bottleneck for maximizing the combinational therapeutic efficacy. In this work, we developed a photoactivatable Pt(IV) prodrug-backboned polymeric nanoparticle system (CNP<sub>PtCP/si(c-fos)</sub>) for light-controlled si(c-fos) delivery and synergistic photoactivated chemotherapy (PACT) and RNA interference (RNAi) on platinum-resistant ovarian cancer (PROC). Upon blue-light irradiation (430 nm), CNP<sub>PtCP/si(c-fos)</sub> generates oxygen-independent N<sub>3</sub><sup>•</sup> with mild oxidation energy for efficient endo/lysosomal escape through N<sub>3</sub><sup>•</sup>-assisted photochemical internalization with less gene deactivation. Thereafter, along with Pt(IV) prodrug activation, CNP<sub>PtCP/si(c-fos)</sub> dissociates to release active Pt(II) and unpack si(c-fos) simultaneously. Both in vitro and in vivo results demonstrated that CNP<sub>PtCP/si(c-fos)</sub> displayed excellent synergistic therapeutic efficacy on PROC with low toxicity. This PACT prodrug-backboned polymeric nanoplatform may provide a promising gene/drug codelivery tactic for treatment of various hard-to-tackle cancers.
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