Enhanced topical delivery of dexamethasone by β-cyclodextrin decorated thermoresponsive nanogels

被引:53
作者
Giulbudagian, M. [1 ]
Hoenzke, S. [2 ]
Bergueiro, J. [1 ]
Isik, D. [1 ]
Schumacher, F. [3 ,6 ]
Saeidpour, S. [4 ]
Lohan, S. B. [5 ]
Meinke, M. C. [5 ]
Teutloff, C. [4 ]
Schaefer-Korting, M. [2 ]
Yealland, G. [2 ]
Kleuser, B. [3 ]
Hedtrich, S. [2 ]
Calderon, M. [1 ]
机构
[1] Free Univ Berlin, Inst Chem & Biochem, Takustr 3, D-14195 Berlin, Germany
[2] Free Univ Berlin, Inst Pharm Pharmacol & Toxicol, Konigin Luise Str 2 4, D-14195 Berlin, Germany
[3] Univ Potsdam, Inst Nutr Sci, Dept Nutr Toxicol, Nuthetal, Germany
[4] Free Univ Berlin, Berlin Joint EPR Lab, Fachbereich Phys, Berlin, Germany
[5] Charite, Dept Dermatol Venerol & Allergol, Ctr Expt & Appl Cutaneous Physiol, Berlin, Germany
[6] Univ Duisburg Essen, Dept Mol Biol, Essen, Germany
关键词
POLYGLYCEROL-BASED NANOGELS; DRUG-DELIVERY; DENDRITIC POLYGLYCEROL; CUTANEOUS DELIVERY; SKIN PENETRATION; BARRIER FUNCTION; IN-VITRO; NANOPARTICLES; NANOCARRIERS; CELLS;
D O I
10.1039/c7nr04480a
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Highly hydrophilic, responsive nanogels are attractive as potential systems for the topical delivery of bioactives encapsulated in their three-dimensional polymeric scaffold. Yet, these drug carrier systems suffer from drawbacks for efficient delivery of hydrophobic drugs. Addressing this, beta-cyclodextrin (beta CD) could be successfully introduced into the drug carrier systems by exploiting its unique affinity toward dexamethasone (DXM) as well as its role as topical penetration enhancer. The properties of beta CD could be combined with those of thermoresponsive nanogels (tNGs) based on dendritic polyglycerol (dPG) as a crosslinker and linear thermoresponsive polyglycerol (tPG) inducing responsiveness to temperature changes. Electron paramagnetic resonance (EPR) studies localized the drug within the hydrophobic cavity of beta CD by differences in its mobility and environmental polarity. In fact, the fabricated carriers combining a particulate delivery system with a conventional penetration enhancer, resulted in an efficient delivery of DXM to the epidermis and the dermis of human skin ex vivo (enhancement compared to commercial DXM cream: similar to 2.5 fold in epidermis, similar to 30 fold in dermis). Furthermore, DXM encapsulated in beta CD tNGs applied to skin equivalents downregulated the expression of proinflammatory thymic stromal lymphopoietin (TSLP) and outperformed a commercially available DXM cream.
引用
收藏
页码:469 / 479
页数:11
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