Melt-electrospinning as a method to improve the dissolution and physical stability of a poorly water-soluble drug
Soluplus (R)
Drug Compounding
Indomethacin
POLYMER MISCIBILITY
EXTRUSION
Pharmacy
02 engineering and technology
Poorly water-soluble drug
SOLUBILITY
DOSAGE FORMS
Melt-spun fibers
Polyethylene Glycols
Drug-polymer interactions
STARCH ACETATES
Drug Stability
AMORPHOUS SOLID DISPERSIONS
SOLUPLUS(R)
Water
STATE
Drug Liberation
Melt electrospinning
INDOMETHACIN
Chemical sciences
Solubility
ORAL BIOAVAILABILITY
Polyvinyls
0210 nano-technology
DOI:
10.1016/j.ejps.2018.06.004
Publication Date:
2018-06-06T08:24:56Z
AUTHORS (10)
ABSTRACT
The present study introduces a modified melt-electrospinning (MES) method for fabricating the melt-electrospun fibers (MSFs) of a poorly water-soluble drug and carrier polymer. The MES of poorly water-soluble model drug indomethacin (IND) and hydrophilic carrier polymer, Soluplus® (SOL) were prepared at a 1:3 drug-polymer weight ratio. Water was used as an external plasticizer to regulate a MES processing temperature and to improve fiber formation. The fiber size, surface morphology, physical solid state, drug-polymer (carrier) interactions, thermal and chemical stability and dissolution behavior of MSFs were investigated. Solid state nuclear magnetic resonance spectroscopy (NMR) was used to measure T1(1H), and the domain size of IND in MSFs (25-100 nm) was calculated from these results. Solid-state and thermal analysis confirmed the presence of amorphous solid dispersions of IND and SOL. IND was found to be chemically stable during an entire MES process. Only small drug content variability of different MSF batches was detected with high performace liquid chromatography (HPLC). Given findings were verified with the liquid NMR spectroscopy. The dissolution of MSFs was significantly faster than that of physical mixtures (PMs) or pure drug. The enhanced dissolution of MSFs was caused by high surface area, amorphous state of the drug and solubilizing properties of the carrier polymer (SOL).
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CITATIONS (13)
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