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PH-Controlled Liposomes for Enhanced Cell Penetration in Tumor Environment

Articolo
Data di Pubblicazione:
2018
Abstract:
An innovative pH-switchable colloidal system that can be exploited for site-selective anticancer drug delivery has been generated by liposome decoration with a new novel synthetic non-peptidic oligo-arginine cell-penetration enhancer (CPE) and a quenching PEGylated counterpart that detaches from the vesicle surface under the acidic conditions of tumors. The CPE module (Arg(4)-DAG) is formed by four arginine units conjugated to a first-generation (G1) 2,2-bis(hydroxymethyl)propionic acid (bis-MPA)/2,2-bis(aminomethyl)propionic acid (bis-AMPA) polyester dendron terminating with 1,2-distearoyl-3-azidopropane for liposome bilayer insertion. The zeta potential of the Arg(4)-DAG-decorated liposomes increased up to +32 mV as the Arg(4)-DAG/lipids molar ratio increased. The Arg(4)-DAG liposome shielding at pH 7.4 was provided by methoxy-PEGS(5 kDa)-polymethacryloyl sulfadimethoxine (mPEG(5) (kDa)-SDM8) with 7.1 apparent pK(a). Zeta potential, surface plasmon resonance and synchrotron small-angle X-ray scattering analyses showed that at pH 7.4 mPEG(5) (kDa)-SDM8 associates with polycationic Arg(4)-DAG-decorated liposomes yielding liposomes with neutral zeta potential. At pH 6.5, which mimics the tumor environment, mPEG(5) (kDa)-SDM8 detaches from the liposome surface yielding Arg(4)-DAG exposure. Flow cytometry and confocal microscopy showed a 30-fold higher HeLa cancer cell association of the Arg(4)-DAG-decorated liposomes compared to non-decorated liposomes. At pH 7.4, the mPEG(5) (kDa)-SDM8-coated liposomes undergo low cell association while remarkable cell association occurred at pH 6.5, which allowed for the controlled intracellular delivery of model macromolecules and small molecules loaded in the liposome under tumor conditions.
Tipologia CRIS:
01.01 - Articolo in rivista
Keywords:
cell penetration enhancers; controlled cell uptake; pH-responsive liposomes; sheddable liposome coating; site-selective drug delivery; Materials Science (all)
Elenco autori:
Barattin, Michela; Mattarei, Andrea; Balasso, Anna; Paradisi, Cristina; Cantù, Laura; Del Favero, Elena; Viitala, Tapani; Mastrotto, Francesca; Caliceti, Paolo; Salmaso, Stefano
Autori di Ateneo:
CALICETI PAOLO
MASTROTTO FRANCESCA
MATTAREI ANDREA
PARADISI CRISTINA
SALMASO STEFANO
Link alla scheda completa:
https://www.research.unipd.it/handle/11577/3276540
Pubblicato in:
ACS APPLIED MATERIALS & INTERFACES
Journal
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URL

http://pubs.acs.org/journal/aamick
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