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- 2018
Augmented tumor accumulation and photothermal ablation using gold nanoparticles with a particular cellular entry orientationKeywords: Gold nanoparticles,one-sided Tat peptide,cellular entry orientation,photothermal tumor ablation,enhanced permeability and retention Abstract: Gold nanoparticles with various functionalities have served as potential tools in nanotechnology for tumor ablation. In this work, we seek to design and develop gold nanoparticle with poly(ethylene glycol)-containing dopamine (hereafter termed as AuND), and to synthesize the AuND with one-sided Tat peptide expression ([email protected]). We demonstrate the tumor cell-targeting ability on the basis of anti-nonspecific cell binding of [email protected] and determine how the chemically modified gold nanoparticle–based product affects photothermal tumor therapy in vitro and in vivo. The [email protected] with a particular cellular entry orientation–induced delayed endocytosis, which is advantageous for enhanced permeability and retention effect-based tumor accumulation. This is because the slower cellular interaction of [email protected] allows it to have the time to be transported to and bind to the tumor site. In tumor cell lines, [email protected] showed a lower cellular uptake than gold nanoparticles with full-sided Tat peptide expression ([email protected]) in the early period (after its in vitro and in vivo administration), but the cellular internalization rate of [email protected] caught up with that of [email protected] in the late period. Importantly, the delayed cellular internalization feature of [email protected] resulted in efficient tumor accumulation in tumor-bearing mice, because the time interval provided [email protected] more chances not to bind to any cells, but to enter tumor cells, leading to selective photothermal tumor ablation. These data suggest that gold nanoparticles with a particular cellular entry orientation can be further explored as a potential photothermal therapeutic agent and as a strategy to treat tumors
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