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Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA

PLGA microspheres undergo physical ageing but their ageing kinetics have not been reported, nor the effect of encapsulated protein or plasmid DNA on any associated changes to the glass transition. Differential scanning calorimetry (DSC) was used to measure the rate of ageing of various PLGAmicrosp...

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Main Authors: Rouse, J. J., Mohamed, Farahidah, van der Walle, Christopher
Format: Article
Language:English
Published: Elsevier Inc. 2007
Subjects:
RS Pharmacy and materia medica
Online Access:http://irep.iium.edu.my/1462/1/physical_ageing_paper_van_der_walle_cf.pdf
http://irep.iium.edu.my/1462/
http://dx.doi.org/10.1016/j.ijpharm.2007.02.026
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spelling my.iium.irep.14622013-01-21T07:30:49Z http://irep.iium.edu.my/1462/ Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA Rouse, J. J. Mohamed, Farahidah van der Walle, Christopher RS Pharmacy and materia medica PLGA microspheres undergo physical ageing but their ageing kinetics have not been reported, nor the effect of encapsulated protein or plasmid DNA on any associated changes to the glass transition. Differential scanning calorimetry (DSC) was used to measure the rate of ageing of various PLGAmicrosphere formulations, with temperature-modulatedDSCused to accurately measure the associated glass transition. The Cowie–Ferguson model was applied to determine the parameters describing the enthalpy relaxation kinetics. We show that encapsulated proteins had no significant effect on the glass transition of the microspheres, whereas DNA and PVA were mild antiplasticising agents, particularly with high Mw PLGA. Physical ageing occurred through a range of enthalpy relaxation times (or modes) and was independent of both encapsulated protein and surfactant used during microsphere preparation. Analysis of accelerated ageing at 35 ◦C gave calculated enthalpy relaxation times to thermal equilibrium of 280–400 h. No ageing was observed ≤10 ◦C and at 25 ◦C estimated relaxation times were at least one order of magnitude greater than at 35 ◦C. Ageing of PLGA microspheres therefore occurs at temperatures >10 ◦C, but relaxation will be far from equilibrium unless storage times and/or temperatures are prolonged or nearing the glass transition, respectively. Elsevier Inc. 2007-02-28 Article REM application/pdf en http://irep.iium.edu.my/1462/1/physical_ageing_paper_van_der_walle_cf.pdf Rouse, J. J. and Mohamed, Farahidah and van der Walle, Christopher (2007) Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA. International Journal of Pharmaceutics, 339 (1-2). pp. 112-120. ISSN 0378-5173 http://dx.doi.org/10.1016/j.ijpharm.2007.02.026 10.1016/j.ijpharm.2007.02.026
institution Universiti Islam Antarabangsa Malaysia
building IIUM Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider International Islamic University Malaysia
content_source IIUM Repository (IREP)
url_provider http://irep.iium.edu.my/
language English
topic RS Pharmacy and materia medica
spellingShingle RS Pharmacy and materia medica
Rouse, J. J.
Mohamed, Farahidah
van der Walle, Christopher
Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA
description PLGA microspheres undergo physical ageing but their ageing kinetics have not been reported, nor the effect of encapsulated protein or plasmid DNA on any associated changes to the glass transition. Differential scanning calorimetry (DSC) was used to measure the rate of ageing of various PLGAmicrosphere formulations, with temperature-modulatedDSCused to accurately measure the associated glass transition. The Cowie–Ferguson model was applied to determine the parameters describing the enthalpy relaxation kinetics. We show that encapsulated proteins had no significant effect on the glass transition of the microspheres, whereas DNA and PVA were mild antiplasticising agents, particularly with high Mw PLGA. Physical ageing occurred through a range of enthalpy relaxation times (or modes) and was independent of both encapsulated protein and surfactant used during microsphere preparation. Analysis of accelerated ageing at 35 ◦C gave calculated enthalpy relaxation times to thermal equilibrium of 280–400 h. No ageing was observed ≤10 ◦C and at 25 ◦C estimated relaxation times were at least one order of magnitude greater than at 35 ◦C. Ageing of PLGA microspheres therefore occurs at temperatures >10 ◦C, but relaxation will be far from equilibrium unless storage times and/or temperatures are prolonged or nearing the glass transition, respectively.
format Article
author Rouse, J. J.
Mohamed, Farahidah
van der Walle, Christopher
author_facet Rouse, J. J.
Mohamed, Farahidah
van der Walle, Christopher
author_sort Rouse, J. J.
title Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA
title_short Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA
title_full Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA
title_fullStr Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA
title_full_unstemmed Physical ageing and thermal analysis of PLGA microspheres encapsulating protein or DNA
title_sort physical ageing and thermal analysis of plga microspheres encapsulating protein or dna
publisher Elsevier Inc.
publishDate 2007
url http://irep.iium.edu.my/1462/1/physical_ageing_paper_van_der_walle_cf.pdf
http://irep.iium.edu.my/1462/
http://dx.doi.org/10.1016/j.ijpharm.2007.02.026
_version_ 1643604795368407040
score 13.209306

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