Preparation of a novel lipid-core micelle using a low-energy emulsification method
Author
dc.contributor.author
Fritz, Hans
Author
dc.contributor.author
Ortiz, Andrea
Author
dc.contributor.author
Velaga, Sitaram
Author
dc.contributor.author
Morales, Javier
Admission date
dc.date.accessioned
2018-12-20T15:11:48Z
Available date
dc.date.available
2018-12-20T15:11:48Z
Publication date
dc.date.issued
2018
Cita de ítem
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Drug Delivery and Translational Research, Volumen 8, Issue 6, 2018, Pages 1807-1814
Identifier
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21903948
Identifier
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2190393X
Identifier
dc.identifier.other
10.1007/s13346-018-0521-9
Identifier
dc.identifier.uri
https://repositorio.uchile.cl/handle/2250/158459
Abstract
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High-energy methods for the manufacturing of nanomedicines are widely used; however, interest in low-energy methods is increasing due to their simplicity, better control over the process, and energy-saving characteristics during upscaling. Here, we developed a novel lipid-core micelle (LCM) as a nanocarrier to encapsulate a poorly water-soluble drug, nifedipine (NFD), by hot-melt emulsification, a low-energy method. LCMs are self-assembling colloidal particles composed of a hydrophobic core and a hydrophilic shell. Hybrid materials, such as Gelucire 44/14, are thus excellent candidates for their preparation. We characterized the obtained nanocarriers for their colloidal properties, drug loading and encapsulation efficiency, liquid state, stability, and drug release. The low-energy method hot-melt emulsification was successfully adapted for the manufacturing of small and narrowly dispersed LCMs. The obtained LCMs had a small average size of ~ 11 nm and a narrow polydispersity index (PDI) of 0.228. These nanocarriers were able to increase the amount of NFD dispersible in water more than 700-fold. Due to their sustained drug release profile and the PEGylation of Gelucire 44/14, these nanocarriers represent an excellent starting point for the development of drug delivery systems designed for long circulation times and passive targeting.