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Rapidly dissolving microneedles for the delivery of cubosome-like liquid crystalline nanoparticles with sustained release of rapamycin
被引:66
作者:

Ramalheiro, Ana
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Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal
Inst Super Tecn, Lisbon, Portugal Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal

Paris, Juan L.
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Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal

Silva, Bruno F. B.
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Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal

Pires, Liliana R.
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Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal
机构:
[1] Int Iberian Nanotechnol Lab INL, Av Mestre Jose Veiga S-N, P-4715330 Braga, Portugal
[2] Inst Super Tecn, Lisbon, Portugal
关键词:
Microneedles;
Rapamycin;
Cubosomes;
Transdermal;
Sustained drug release;
INFLUENZA VACCINE;
CUBIC PHASE;
NATURAL-KILLER;
DRUG;
PATHOGENESIS;
TRANSITION;
STABILITY;
CARRIERS;
LENGTH;
F127;
D O I:
10.1016/j.ijpharm.2020.119942
中图分类号:
R9 [药学];
学科分类号:
1007 ;
摘要:
In this study, we developed a system for the transdermal delivery and controlled release of the hydrophobic immunosuppressive drug rapamycin, foreseeing an application in psoriasis treatment. To do so, rapamycin was encapsulated in phytantriol-based cubosome-like liquid crystalline nanoparticles stabilized with plumnic F127. The final mass percent composition of the lipid nanoparticles was 0.25% phytantriol, 0.1% plumnic F127, 4.75% ethanol and 94.9% water. These particles showed a rapamycin encapsulation efficiency above 95% and a sustained in vitro drug release profile throughout 14 days. Subsequently the rapamycin-carrying particles were incorporated into rapidly dissolving microneedle patches composed of a polymeric matrix of poly(vinylpyrrolidone) and poly(vinyl alcohol). Confocal microscopy allowed to infer the preferential distribution of the cubosome-like particles at the tip and baseplate of the microneedles. The fabricated microneedles showed successful piercing and deposition of the loaded cubosome-like particles on a skin-mimicking agamse gel. Finally, the rapamycin-loaded cubosome-like particles showed antiproliferative activity in natural killer cells in vitro. The results here presented show the potential of the developed system to deliver cubosome-like particles into the skin and promote the sustained release of rapamycin in the context of immunomodulation.
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