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Micro-syringe chip-guided intratumoral administration of lipid nanoparticles for targeted anticancer therapy.

Jeongrae KimSunejeong SongMinjun GwakHanhee ChoWan Su YunNamcheol HwangJinseong KimJun Seo LeeDong-Hwee KimHyuncheol KimSeong Ik JeonTae-Il KimKwangmeyung Kim
Published in: Biomaterials research (2023)
The MSC-guided administration of LNPs greatly enhances the therapeutic efficiency of anticancer drugs via the slow diffusion mechanism through micro-syringe to tumor tissues for 6 h, whereas they bypass most hurdles of systemic delivery including hepatic metabolism, rapid renal clearance, and interaction with blood components or other normal tissues, resulting in the minimum toxicity to normal tissues. The negatively charged ApoLNPs with cancer cell-specific pro-apoptotic prodrug (SMAC-P-FRRG-DOX) show the highest tumor-targeting efficacy when they are treated with the MSC guidance, compared to their intravenous or intratumoral administration in 4T1 tumor-bearing mice. The MSC-guided administration of anticancer drug-encapsulated LNPs is expected to be a potent platform system that facilitates overcoming the limitations of systemic drug administration with low delivery efficiency and serious side effects.
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