Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets

Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets

Cilostazol was selected as poorly-soluble model drug to investigate the impact of the manufacturing method on the excipient functionality of PEG4000 at various levels. Powder blends were prepared by direct compression (DC), wet granulation (WG) and hot-melt extrusion (HME). Character...

Full description

Bibliographic Details
Main Authors: Obada Sawafta, Sonia Alhadid, Izz Aldeen Abu Awwad, Eman Migdadi, Ahmad Aljaberi
Format: Article
Language:English
Published: Pensoft Publishers 2021-02-01
Series:Pharmacia
Online Access:https://pharmacia.pensoft.net/article/62465/download/pdf/
id doaj-86c91717c11049c482d61c3d6a07c1c3
record_format Article
spelling doaj-86c91717c11049c482d61c3d6a07c1c32021-09-28T14:39:05ZengPensoft PublishersPharmacia2603-557X2021-02-0168124325010.3897/pharmacia.68.e6246562465Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tabletsObada Sawafta0Sonia Alhadid1Izz Aldeen Abu Awwad2Eman Migdadi3Ahmad Aljaberi4Applied Science Private UniversityApplied Science Private UniversityTabuk Pharmaceutical Research CompanyApplied Science Private UniversityApplied Science Private University Cilostazol was selected as poorly-soluble model drug to investigate the impact of the manufacturing method on the excipient functionality of PEG4000 at various levels. Powder blends were prepared by direct compression (DC), wet granulation (WG) and hot-melt extrusion (HME). Characteristics of these blends and their compressed tablets were investigated by standard techniques. Solid-state characterization was carried out using differential scanning calorimetry (DSC). While DC trials were found with no significant differences, WG and HME showed contrasting enhancement and retardation effects regarding the dissolution profile of Cilostazol tablets depending on the level of PEG4000 incorporated. The optimal enhancement of dissolution was obtained at 10% w/w PEG4000 for tablets prepared by HME. DSC analysis indicated that no solid solutions were formed at such low levels of PEG4000during processing by either manufacturing techniques. Consequently, the wetting functionality and dissolution enhancement of PEG4000 was revealed to be level- and manufacturing method dependent. https://pharmacia.pensoft.net/article/62465/download/pdf/
collection DOAJ
language English
format Article
sources DOAJ
author Obada Sawafta
Sonia Alhadid
Izz Aldeen Abu Awwad
Eman Migdadi
Ahmad Aljaberi
spellingShingle Obada Sawafta
Sonia Alhadid
Izz Aldeen Abu Awwad
Eman Migdadi
Ahmad Aljaberi
Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets
Pharmacia
author_facet Obada Sawafta
Sonia Alhadid
Izz Aldeen Abu Awwad
Eman Migdadi
Ahmad Aljaberi
author_sort Obada Sawafta
title Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets
title_short Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets
title_full Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets
title_fullStr Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets
title_full_unstemmed Impact of the manufacturing technique on the dissolution-enhancement functionality of PEG4000 in Cilostazol tablets
title_sort impact of the manufacturing technique on the dissolution-enhancement functionality of peg4000 in cilostazol tablets
publisher Pensoft Publishers
series Pharmacia
issn 2603-557X
publishDate 2021-02-01
description Cilostazol was selected as poorly-soluble model drug to investigate the impact of the manufacturing method on the excipient functionality of PEG4000 at various levels. Powder blends were prepared by direct compression (DC), wet granulation (WG) and hot-melt extrusion (HME). Characteristics of these blends and their compressed tablets were investigated by standard techniques. Solid-state characterization was carried out using differential scanning calorimetry (DSC). While DC trials were found with no significant differences, WG and HME showed contrasting enhancement and retardation effects regarding the dissolution profile of Cilostazol tablets depending on the level of PEG4000 incorporated. The optimal enhancement of dissolution was obtained at 10% w/w PEG4000 for tablets prepared by HME. DSC analysis indicated that no solid solutions were formed at such low levels of PEG4000during processing by either manufacturing techniques. Consequently, the wetting functionality and dissolution enhancement of PEG4000 was revealed to be level- and manufacturing method dependent.
url https://pharmacia.pensoft.net/article/62465/download/pdf/
work_keys_str_mv AT obadasawafta impactofthemanufacturingtechniqueonthedissolutionenhancementfunctionalityofpeg4000incilostazoltablets
AT soniaalhadid impactofthemanufacturingtechniqueonthedissolutionenhancementfunctionalityofpeg4000incilostazoltablets
AT izzaldeenabuawwad impactofthemanufacturingtechniqueonthedissolutionenhancementfunctionalityofpeg4000incilostazoltablets
AT emanmigdadi impactofthemanufacturingtechniqueonthedissolutionenhancementfunctionalityofpeg4000incilostazoltablets
AT ahmadaljaberi impactofthemanufacturingtechniqueonthedissolutionenhancementfunctionalityofpeg4000incilostazoltablets
_version_ 1716865568331530240

Similar Items