| Literature DB >> 31078049 |
Hong Cheng1, Jing-Hao Fan2, Lin-Ping Zhao2, Gui-Ling Fan2, Rong-Rong Zheng2, Xiao-Zhong Qiu1, Xi-Yong Yu3, Shi-Ying Li4, Xian-Zheng Zhang5.
Abstract
Targeted delivery of the drug to its therapeutically active site with low immunogenicity and system toxicity is critical for optimal tumor therapy. In this paper, exosomes as naturally-derived nano-sized membrane vesicles are engineered by chimeric peptide for plasma membrane and nucleus targeted photosensitizer delivery and synergistic photodynamic therapy (PDT). Importantly, a dual-stage light strategy is adopted for precise PDT by selectively and sequentially destroying the plasma membrane and nucleus of tumor cells. Briefly, plasma membrane-targeted PDT of chimeric peptide engineered exosomes (ChiP-Exo) could directly disrupt the membrane integrity and cause cell death to some extent. More interestingly, the photochemical internalization (PCI) and lysosomal escape triggered by the first-stage light significantly improve the cytosolic delivery of ChiP-Exo, which could enhance its nuclear delivery due to the presence of nuclear localization signals (NLS) peptide. Upon the second-stage light irradiation, the intranuclear ChiP-Exo would activate reactive oxygen species (ROS) in situ to disrupt nuclei for robust and synergistic PDT. Based on exosomes, this dual-stage light guided subcellular dual-targeted PDT strategy exhibits a greatly enhanced therapeutic effect on the inhibition of tumor growth with minimized system toxicity, which also provides a new insight for the development of individualized biomedicine for precise tumor therapy.Entities:
Keywords: Dual-targeting; Exosomes; Lysosomal escape; Photochemical internalization; Photodynamic therapy
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Year: 2019 PMID: 31078049 DOI: 10.1016/j.biomaterials.2019.05.004
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479