| Literature DB >> 28795851 |
Cristina Minnelli1, Laura Cianfruglia2, Emiliano Laudadio1, Roberta Galeazzi1, Michela Pisani3, Emanuela Crucianelli1, Davide Bizzaro1, Tatiana Armeni2, Giovanna Mobbili1.
Abstract
Liposomes are versatile platforms to carry anticancer drugs in targeted drug delivery; they can be surface modified by different strategies and, when coupled with targeting ligands, are able to increase cellular internalisation and organelle-specific drug delivery. An interesting strategy of antitumoral therapy could involve the use of lysosomotropic ligand-targeted liposomes loaded with molecules, which can induce lysosomal membrane permeabilization (LMP), leakage of cathepsins into the cytoplasm and subsequent apoptosis. We have previously demonstrated the ability of liposomes functionalised with a mannose-6-phosphate to reach lysosomes; in this research we compare the behaviour of M6P-modified and non-functionalised liposomes in MCF7 tumour cell and in HDF normal cells. With this aim, we first demonstrated by Western blotting the overexpression of mannose-6-phosphate/insulin-like growth factor (M6P/IGF-II) receptor in MCF7. Then, we prepared calcein-loaded liposomes and we revealed the increased uptake of M6P-functionalised liposomes in MCF7 cells respect to HDF cells by flow cytometry analysis. Finally, we loaded functionalised and not functionalised liposomes with N-hexanoyl-d-erythro-sphingosine (C6Cer), able to initiate LMP-induced apoptosis; after having studied the stability of both vesicles in the presence of serum by Dynamic Light Scattering and Spectrophotometric turbidity measurements, we showed that ceramide-loaded M6P-liposomes significantly increased apoptosis in MCF7 with respect to HDF cells.Entities:
Keywords: Targeted drug delivery; apoptosis; cancer therapy; ceramide; liposomes; mannose-6-phosphate/insulin-like growth factor (M6P/IGF-II) receptor
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Year: 2017 PMID: 28795851 DOI: 10.1080/1061186X.2017.1365873
Source DB: PubMed Journal: J Drug Target ISSN: 1026-7158 Impact factor: 5.121