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Solvent-Mediated Polymorphic Transformations in Molten Polymers: The Account of Acetaminophen.

José R Hernández EspinellVerónica ToroXin YaoLian YuVilmalí López-MejíasTorsten Stelzer
Published in: Molecular pharmaceutics (2022)
Solvent-mediated polymorphic transformations (SMPTs) employing nonconventional solvents (polymer melts) is an underexplored research topic that limits the application of polymer-based formulation processes. Acetaminophen (ACM), a widely studied active pharmaceutical ingredient (API), is known to present SMPTs spontaneously (<30 s) in conventional solvents such as ethanol. In situ Raman spectroscopy was employed to monitor the induction time for the SMPT of ACM II to I in polyethylene glycol (PEG) melts of different molecular weights ( M w , 4000, 10 000, 20 000, 35 000 g/mol). The results presented here demonstrate that the induction time for the SMPT of ACM II to I in PEG melts is driven by its diffusivity through the polymer melts. Compared to conventional solvents ( i.e. , ethanol) the mass transfer (diffusion coefficient, D ) in melts is significantly hindered ( D ethanol = 4.84 × 10 -9 m 2 /s > D PEGs = 5.32 × 10 -11 -8.36 × 10 -14 m 2 /s). Ultimately, the study proves that the induction time for the SMPT can be tuned by understanding the dispersant's physicochemical properties ( i.e. , η) and, thus, the D of the solute in the dispersant. This allows one to kinetically access and stabilize metastable forms or delay their transformations under given process conditions.
Keyphrases
  • ionic liquid
  • raman spectroscopy
  • drug delivery
  • liver injury
  • computed tomography
  • magnetic resonance