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Investigating phase separation in amorphous solid dispersions via Raman mapping
Authors:Christian Luebbert  Christian Klanke  Gabriele Sadowski
Affiliation:Department of Biochemical and Chemical Engineering, Laboratory of Thermodynamics, TU Dortmund University, Emil-Figge-Str. 70, D-44227 Dortmund, Germany
Abstract:The bioavailability of poorly-water-soluble active pharmaceutical ingredients (APIs) can be significantly improved by so-called amorphous solid dispersions (ASDs). However, the long-term stability of ASDs might be impaired by API recrystallization and/or amorphous phase separation (APS). So far, no methods have been reported to quantify APS in ASDs. In this work, phase-separation kinetics as well as the compositions of the two amorphous phases evolving due to APS were quantitatively determined for the first time using confocal Raman spectroscopy. Raman spectra were evaluated via non-linear multivariate Indirect Hard Modeling and verified by differential scanning calorimetry and hot-stage microscopy. APS in water-free ASDs of ibuprofen and poly (DL-lactic-co-glycolic acid) was investigated considering the influence of temperature and polymer architecture (linear vs. star-shaped). Water absorbed at 40?°C and 75% relative humidity (RH) promotes APS which was quantified for formulations of felodipine/poly(vinyl pyrrolidone) and ibuprofen/poly(vinyl pyrrolidone).
Keywords:API  active pharmaceutical ingredient  APS  amorphous-amorphous phase separation  ASD  amorphous solid dispersion  DSC  differential scanning calorimetry  FEL  felodipine  GA  glycolic acid  HSM  hot-stage microscopy  IBU  ibuprofen  IHM  Indirect Hard Modeling  LA  lactic acid  M  molecular weight  MIAPS  moisture-induced amorphous-amorphous phase separation  PG  hyperbranched poly glycerol  PLGA  RH  relative humidity  T  temperature  w  weight fraction  Amorphous solid dispersion  Water sorption  Poorly-soluble drug  Amorphous-amorphous phase separation  Long-term stability  Confocal Raman spectroscopy  Indirect Hard Modeling
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