| Literature DB >> 29248674 |
Maria Manconi1, Maria Letizia Manca2, Carla Caddeo1, Donatella Valenti1, Claudia Cencetti3, Octavio Diez-Sales4, Amparo Nacher4, Silvia Mir-Palomo4, Maria Carmen Terencio5, Davide Demurtas6, Juan Carmelo Gomez-Fernandez7, Francisco José Aranda7, Anna Maria Fadda1, Pietro Matricardi3.
Abstract
Gellan nanohydrogel and phospholipid vesicles were combined to incorporate baicalin in new self-assembling core-shell gellan-transfersomes obtained by an easy, scalable method. The vesicles were small in size (~107 nm) and monodispersed (P.I. ≤ 0.24), forming a viscous system (~24 mPa/s) as compared to transfersomes (~1.6 mPa/s), as confirmed by rheological studies. Gellan was anchored to the bilayer domains through cholesterol, and the polymer chains were distributed onto the outer surface of the bilayer, thus forming a core-shell structure, as suggested by SAXS analyses. The optimal carrier ability of core-shell gellan-transfersomes was established by the high deposition of baicalin in the skin (~11% in the whole skin), especially in the deeper tissue (~8% in the dermis). Moreover, their ability to improve baicalin efficacy in anti-inflammatory and skin repair tests was confirmed in vivo in mice, providing the complete skin restoration and inhibiting all the studied inflammatory markers.Entities:
Keywords: Gellan; In vivo studies; Rheological studies; SAXS analysis; Skin delivery; Transfersomes
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Year: 2017 PMID: 29248674 DOI: 10.1016/j.nano.2017.12.001
Source DB: PubMed Journal: Nanomedicine ISSN: 1549-9634 Impact factor: 5.307