Literature DB >> 33498609

How Does the Addition of Kollidon®VA64 Inhibit the Recrystallization and Improve Ezetimibe Dissolution from Amorphous Solid Dispersions?

Joanna Szafraniec-Szczęsny1,2, Agata Antosik-Rogóż1, Mateusz Kurek1, Karolina Gawlak2, Anna Górska1, Sebastian Peralta3, Justyna Knapik-Kowalczuk4, Daniel Kramarczyk4, Marian Paluch4, Renata Jachowicz1.   

Abstract

Amorphization serves as a strategy for the improvement of poor dissolution characteristics of many drug compounds. However, in many formulations the content of polymeric stabilizer is high, which is undesirable from the perspective of future applications. Thus, studying the composition-dependent stability of amorphous solid dispersions seems to be demanded. In this paper, we describe the amorphization of ezetimibe, a lipid-lowering drug, in the spray drying process and investigate the effect of polyvinylpyrrolidone-co-poly(vinyl acetate) (PVP/VA) content on the physical stability and dissolution characteristics of the drug. Fully amorphous systems were obtained when the concentration of the polymer in solid dispersion was as low as 20%. The amorphization led to the dissolution enhancement by even 70%, with a noticeable sudden increase at around 40% of PVP/VA content and very small variations for systems having 66-90% PVP/VA. It was also correlated to wettability characteristics of solid dispersions, which may suggest that in the vicinity of 40% of the polymer content, the behavior of the system becomes independent of the PVP/VA content.

Entities:  

Keywords:  amorphization; contact angle; dissolution; ezetimibe; solid dispersion

Year:  2021        PMID: 33498609      PMCID: PMC7912050          DOI: 10.3390/pharmaceutics13020147

Source DB:  PubMed          Journal:  Pharmaceutics        ISSN: 1999-4923            Impact factor:   6.321


  38 in total

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