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HII mesophase and peptide cell-penetrating enhancers for improved transdermal delivery of sodium diclofenac
Institution:1. Laboratory of Physical Chemistry, Department of Pharmacy, Faculty of Pharmacy, Yasuda Women''s University, 6-13-1, Yasuhigashi, Asaminami-ku, Hiroshima-shi, Hiroshima 731-0153, Japan;2. Laboratory of Physical Chemistry, Department of Pharmacy, Faculty of Pharmacy, Yasuda Women’s University, 6-13-1, Yasuhigashi, Asaminami-ku, Hiroshima-shi, Hiroshima 731-0153, Japan;3. Laboratory of Medical Pharmaceutics, Department of Pharmacy, Faculty of Pharmacy, Yasuda Women''s University, 6-13-1, Yasuhigashi, Asaminami-ku, Hiroshima-shi, Hiroshima 731-0153, Japan
Abstract:This study develops a novel transdermal delivery vehicle for the enhanced delivery of sodium diclofenac (Na-DFC). The system utilizes the advantages of reversed hexagonal lyotropic liquid crystals (HIILC), combined with a peptide cell penetration enhancer (CPE), creating together an adaptable system that provides versatile options in the field of transdermal delivery.This enhancer peptide is based on a family of amphipatic peptides that exhibit improved membrane permeability. Franz permeation cell experiments revealed that the peptide enhancer (RALA) improved Na-DFC skin penetration of the liquid crystal 2.2-fold.We studied the structural effects of RALA solubilization on the HII mesophase. RALA acts as a chaotropic agent, interfering in the structure of the water, and causes a measurable swelling of the aqueous cylinders by 5 Å.Small angle X-ray scattering (SAXS) and attenuated total reflectance–Fourier transform infrared (ATR–FTIR) measurements reveal enhanced hydration of the glycerol monooleate (GMO) headgroups and a 6.5% increase in the fraction of non-freezable water resulting from RALA incorporation. RALA caused a gradual increase in the GMO effective headgroup area due to the hydration, leading eventually to a transform of the hexagonal structure towards a lamellar one. Circular dichroism and ATR–FTIR measurements showed a conservation of the peptide structure when incorporated into the HII mesophase.The combined HIILC-CPE systems can serve as high potential vehicles for a variety of drugs, as they can easily be modified by varying the composition and temperature, according to the required dose and delivery features.
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