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Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound

The main purpose of this paper was to evaluate the impact of both high- and low-T(g) polymer additives on the physical stability of an amorphous drug, sildenafil (SIL). The molecular mobility of neat amorphous SIL was strongly affected by the polymeric excipients used (Kollidon VA64 (KVA) and poly(v...

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Autores principales: Knapik-Kowalczuk, Justyna, Chmiel, Krzysztof, Pacułt, Justyna, Bialek, Klaudia, Tajber, Lidia, Paluch, Marian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7284710/
https://www.ncbi.nlm.nih.gov/pubmed/32443637
http://dx.doi.org/10.3390/pharmaceutics12050460
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author Knapik-Kowalczuk, Justyna
Chmiel, Krzysztof
Pacułt, Justyna
Bialek, Klaudia
Tajber, Lidia
Paluch, Marian
author_facet Knapik-Kowalczuk, Justyna
Chmiel, Krzysztof
Pacułt, Justyna
Bialek, Klaudia
Tajber, Lidia
Paluch, Marian
author_sort Knapik-Kowalczuk, Justyna
collection PubMed
description The main purpose of this paper was to evaluate the impact of both high- and low-T(g) polymer additives on the physical stability of an amorphous drug, sildenafil (SIL). The molecular mobility of neat amorphous SIL was strongly affected by the polymeric excipients used (Kollidon VA64 (KVA) and poly(vinylacetate) (PVAc)). The addition of KVA slowed down the molecular dynamics of amorphous SIL (antiplasticizing effect), however, the addition of PVAc accelerated the molecular motions of the neat drug (plasticizing effect). Therefore, in order to properly assess the effect of the polymer on the physical stability of SIL, the amorphous samples at both: isothermal (at constant temperature—353 K) and isochronal (at constant relaxation time—τ(α) = 1.5 ms) conditions were compared. Our studies showed that KVA suppressed the recrystallization of amorphous SIL more efficiently than PVAc. KVA improved the physical stability of the amorphous drug, regardless of the chosen concentration. On the other hand, in the case of PVAc, a low polymer content (i.e., 25 wt.%) destabilized amorphous SIL, when stored at 353 K. Nevertheless, at high concentrations of this excipient (i.e., 75 wt.%), its effect on the amorphous pharmaceutical seemed to be the opposite. Therefore, above a certain concentration, the PVAc presence no longer accelerates the SIL recrystallization process, but inhibits it.
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spelling pubmed-72847102020-06-15 Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound Knapik-Kowalczuk, Justyna Chmiel, Krzysztof Pacułt, Justyna Bialek, Klaudia Tajber, Lidia Paluch, Marian Pharmaceutics Article The main purpose of this paper was to evaluate the impact of both high- and low-T(g) polymer additives on the physical stability of an amorphous drug, sildenafil (SIL). The molecular mobility of neat amorphous SIL was strongly affected by the polymeric excipients used (Kollidon VA64 (KVA) and poly(vinylacetate) (PVAc)). The addition of KVA slowed down the molecular dynamics of amorphous SIL (antiplasticizing effect), however, the addition of PVAc accelerated the molecular motions of the neat drug (plasticizing effect). Therefore, in order to properly assess the effect of the polymer on the physical stability of SIL, the amorphous samples at both: isothermal (at constant temperature—353 K) and isochronal (at constant relaxation time—τ(α) = 1.5 ms) conditions were compared. Our studies showed that KVA suppressed the recrystallization of amorphous SIL more efficiently than PVAc. KVA improved the physical stability of the amorphous drug, regardless of the chosen concentration. On the other hand, in the case of PVAc, a low polymer content (i.e., 25 wt.%) destabilized amorphous SIL, when stored at 353 K. Nevertheless, at high concentrations of this excipient (i.e., 75 wt.%), its effect on the amorphous pharmaceutical seemed to be the opposite. Therefore, above a certain concentration, the PVAc presence no longer accelerates the SIL recrystallization process, but inhibits it. MDPI 2020-05-18 /pmc/articles/PMC7284710/ /pubmed/32443637 http://dx.doi.org/10.3390/pharmaceutics12050460 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Knapik-Kowalczuk, Justyna
Chmiel, Krzysztof
Pacułt, Justyna
Bialek, Klaudia
Tajber, Lidia
Paluch, Marian
Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound
title Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound
title_full Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound
title_fullStr Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound
title_full_unstemmed Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound
title_short Enhancement of the Physical Stability of Amorphous Sildenafil in a Binary Mixture, with either a Plasticizing or Antiplasticizing Compound
title_sort enhancement of the physical stability of amorphous sildenafil in a binary mixture, with either a plasticizing or antiplasticizing compound
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7284710/
https://www.ncbi.nlm.nih.gov/pubmed/32443637
http://dx.doi.org/10.3390/pharmaceutics12050460
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