Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design
Context: High melting point polymeric carrier without plasticizer is unacceptable for solid dispersion (SD) by melting method. Combined polymer–plasticizer carrier significantly affects drug solubility and tableting property of SD. Objective: To evaluate and optimize the combined effect of a bina...
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Taylor and Francis
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iium-460582018-01-19T03:03:29Z http://irep.iium.edu.my/46058/ Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design Kyaw Oo, May Mandal, Uttam Kumar Chatterjee, Bappaditya RS Pharmacy and materia medica Context: High melting point polymeric carrier without plasticizer is unacceptable for solid dispersion (SD) by melting method. Combined polymer–plasticizer carrier significantly affects drug solubility and tableting property of SD. Objective: To evaluate and optimize the combined effect of a binary carrier consisting PVP K30 and poloxamer 188, on nisoldipine solubility and tensile strength of amorphous SD compact (SDcompact) by experimental design. Materials and methods: SD of nisoldpine (SDnisol) was prepared by melt mixing with different PVP K30 and poloxamer amount. A 32 factorial design was employed using nisoldipine solubility and tensile strength of SDcompact as response variables. Statistical optimization by design expert software, and SDnisol characterization using ATR FTIR, DSC and microscopy were done. Results: PVP K30:poloxamer, at a ratio of 3.73:6.63, was selected as the optimized combination of binary polymeric carrier resulting nisoldipine solubility of 115 mg/mL and tensile strength of 1.19 N/m2 . Discussion: PVP K30 had significant positive effect on both responses. Increase in poloxamer concentration after a certain level decreased nisoldipine solubility and tensile strength of SDcompact. Conclusion: An optimized PVP K30–poloxamer binary composition for SD carrier was developed. Tensile strength of SDcompact can be considered as a response for experimental design to optimize SD. Taylor and Francis 2015 Article PeerReviewed application/pdf en http://irep.iium.edu.my/46058/1/published_copy.pdf application/pdf en http://irep.iium.edu.my/46058/4/Polymeric%20behavior%20evaluation%20of%20PVP%20K30-%20poloxamer%20binary%20carrier%20for%20solid%20dispersed%20nisoldipine%20by%20experimental%20design.pdf Kyaw Oo, May and Mandal, Uttam Kumar and Chatterjee, Bappaditya (2015) Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design. Pharmaceutical Development Technology. pp. 1-11. ISSN 1083-7450 (P) 1097-9867 (O) (In Press) http://www.tandfonline.com/loi/iphd20#.VmeMT_l97IU |
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RS Pharmacy and materia medica Kyaw Oo, May Mandal, Uttam Kumar Chatterjee, Bappaditya Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
description |
Context: High melting point polymeric carrier without plasticizer is unacceptable for solid
dispersion (SD) by melting method. Combined polymer–plasticizer carrier significantly affects
drug solubility and tableting property of SD.
Objective: To evaluate and optimize the combined effect of a binary carrier consisting PVP K30
and poloxamer 188, on nisoldipine solubility and tensile strength of amorphous SD compact
(SDcompact) by experimental design.
Materials and methods: SD of nisoldpine (SDnisol) was prepared by melt mixing with different
PVP K30 and poloxamer amount. A 32 factorial design was employed using nisoldipine
solubility and tensile strength of SDcompact as response variables. Statistical optimization by
design expert software, and SDnisol characterization using ATR FTIR, DSC and microscopy were
done.
Results: PVP K30:poloxamer, at a ratio of 3.73:6.63, was selected as the optimized combination
of binary polymeric carrier resulting nisoldipine solubility of 115 mg/mL and tensile strength of
1.19 N/m2
.
Discussion: PVP K30 had significant positive effect on both responses. Increase in poloxamer
concentration after a certain level decreased nisoldipine solubility and tensile strength of
SDcompact.
Conclusion: An optimized PVP K30–poloxamer binary composition for SD carrier was developed.
Tensile strength of SDcompact can be considered as a response for experimental design to
optimize SD. |
format |
Article |
author |
Kyaw Oo, May Mandal, Uttam Kumar Chatterjee, Bappaditya |
author_facet |
Kyaw Oo, May Mandal, Uttam Kumar Chatterjee, Bappaditya |
author_sort |
Kyaw Oo, May |
title |
Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
title_short |
Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
title_full |
Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
title_fullStr |
Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
title_full_unstemmed |
Polymeric behavior evaluation of PVP K30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
title_sort |
polymeric behavior evaluation of pvp k30- poloxamer binary carrier for solid dispersed nisoldipine by experimental design |
publisher |
Taylor and Francis |
publishDate |
2015 |
url |
http://irep.iium.edu.my/46058/ http://irep.iium.edu.my/46058/ http://irep.iium.edu.my/46058/1/published_copy.pdf http://irep.iium.edu.my/46058/4/Polymeric%20behavior%20evaluation%20of%20PVP%20K30-%20poloxamer%20binary%20carrier%20for%20solid%20dispersed%20nisoldipine%20by%20experimental%20design.pdf |
first_indexed |
2023-09-18T21:05:33Z |
last_indexed |
2023-09-18T21:05:33Z |
_version_ |
1777410908482437120 |