| Literature DB >> 29058908 |
Li Ding1,2, Xianbing Zhu1,2, Yiling Wang1,2, Bingyang Shi3, Xiang Ling4, Houjie Chen1,2, Wenhao Nan1,2, Austin Barrett5, Zilei Guo5, Wei Tao1,2,5, Jun Wu4, Xiaojun Shi1,2.
Abstract
Polydopamine (PDA) coating as a bioinspired strategy for nanoparticles (NPs) has been extensively applied in cancer theranostics. However, a cellular-level understanding of nano-biointeraction of these PDA-coated NPs (PDNPs), which drives the fate of them and acts as a critical step to determine their efficacy, still remains unknown. Herein, we utilized the representative mesoporous silica NPs (MSNs) to be coated with PDA and study their nano-bioactivities in cancer cells. HeLa cell line was utilized as a model in this study. The PDNPs were discovered to be internalized through three specific pathways, that is, Caveolae-, Arf6-dependent endocytosis, and Rab34-mediated macropinocytosis (55%, 20% and 37% of uptake inhibition by nystatin, Arf6 knockdown, and rottlerin, respectively). Autophagy-mediated accumulation of PDNPs in lysosomes was observed and the formed PDA shells shedded in the lysosomes. Almost 40% of the NPs were transported out of cells via Rab8/10- and Rab3/26-mediated exocytosis pathways at our tested level. On the basis of these results, a novel combined cancer treatment strategy was further proposed using drug-loaded MSNs-PDA by (i) utilizing naturally intracellular mechanism-controlled PDA shedding for organelle-targeted release of drugs in lysosomes to generate lysosome impairment and (ii) blocking the demonstrated exocytosis pathways for enhanced therapeutic efficacy.Entities:
Keywords: Nanoparticle; exocytosis-inhibiting; intracellular fate; lysosome targeting; polydopamine coating and shedding
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Year: 2017 PMID: 29058908 DOI: 10.1021/acs.nanolett.7b03021
Source DB: PubMed Journal: Nano Lett ISSN: 1530-6984 Impact factor: 12.262