Design and evaluation of orally disintegrating tablet containing fixed dose combinations

DC Field Value Language
dc.contributor.advisor이범진-
dc.contributor.author원한나-
dc.date.accessioned2022-11-29T02:31:57Z-
dc.date.available2022-11-29T02:31:57Z-
dc.date.issued2018-02-
dc.identifier.other27427-
dc.identifier.urihttps://dspace.ajou.ac.kr/handle/2018.oak/19434-
dc.description학위논문(석사)--아주대학교 일반대학원 :약학과,2018. 2-
dc.description.tableofcontents1. Introduction 2. Materials and Methods 2.1. Materials 2.2. Preparation of DEX formulations 2.2.1. The effect of method and carrier on content uniformity 2.2.2. The effect of carrier ratio on content uniformity 2.2.3. The effect of taste masking agent and ratio on taste making 2.3. Content uniformity study 2.4. In vitro taste masking evaluation (E-tongue) 2.5. In vitro dissolution study in gastric condition 2.6. Preparation of OND SR granules 2.6.1. Screening of melt binder for OND sustained release 2.6.2. The effect of melt binder ratio on OND sustained release 2.7. In vitro dissolution study in pH shifting condition 2.8. Compatibility study 2.9. ODT preparation containing DEX formulation and OND granule 2.9.1 Screening of cushioning agent 2.9.2 Optimization of in vitro disintegration time 2.10. Characterizations of DEX formulation and OND granule 2.10.1. Differential scanning calorimetry (DSC) 2.10.2. Powder X-ray diffraction (PXRD) 2.10.3. Scanning electron microscopy (SEM) 2.10.4. Powder properties 2.10.5. Stability study 2.11. Physicochemical properties measurements of ODTs 2.11.1. Physical properties measurements of ODTs 2.11.2. Comparison of dissolution profiles by similarity factor (f2) 2.11.3. In vitro disintegration study 2.11.4. Wetting time 2.12. HPLC analysis 3. Results and discussions 3.1. Evaluation of DEX formulations 3.1.1. The effect of method and carrier on content uniformity 3.1.2. The effect of carrier ratio on content uniformity 3.1.3. The effect of taste masking agent and ratio on taste making 3.1.4. Dissolution behavior in gastric condition 3.2. Evaluation of OND SR granules 3.2.1. Screening of melt binder for OND sustained release 3.2.2. The effect of melt binder ratio on SR in pH shift condition 3.3. Characterization of DEX formulation and OND SR granule 3.3.1. Differential scanning calorimetry (DSC) 3.3.2. Powder X-ray diffraction (PXRD) 3.3.3. Scanning electron microscopy (SEM) 3.3.4. Powder properties 3.3.5. Stability study 3.4. Compatibility study 3.5. Physicochemical properties of ODTs 3.5.1. Physical properties of ODTs 3.5.2. Screening of cushioning agent 3.5.3. Optimization of in vitro disintegration time of ODT 3.5.4. Wetting time 3.5.5. The effect of the disintegrant amount on dissolution profile 4. Conclusions 5. References 국문초록-
dc.language.isoeng-
dc.publisherThe Graduate School, Ajou University-
dc.rights아주대학교 논문은 저작권에 의해 보호받습니다.-
dc.titleDesign and evaluation of orally disintegrating tablet containing fixed dose combinations-
dc.title.alternativeDesign and evaluation of orally disintegrating tablet containing fixed dose combinations-
dc.typeThesis-
dc.contributor.affiliation아주대학교 일반대학원-
dc.contributor.department일반대학원 약학과-
dc.date.awarded2018. 2-
dc.description.degreeMaster-
dc.identifier.localId800897-
dc.identifier.urlhttp://dcoll.ajou.ac.kr:9080/dcollection/jsp/common/DcLoOrgPer.jsp?sItemId=000000027427-
dc.subject.keywordcontent uniformity-
dc.subject.keyworddexamethasone-
dc.subject.keywordfixed dose combination-
dc.subject.keywordondansetron-
dc.subject.keywordorally disintegrating tablet-
dc.subject.keywordsustained release-
dc.subject.keywordtaste masking-
dc.description.alternativeAbstractThe objective of this study is to develop a fixed dose combination orally disintegrating tablet (FDC ODT) containing dexamethasone (DEX) formulation with improved content uniformity and taste masking property and ondansetron HCl (OND) sustained release (SR) granule for once daily dosing. The DEX formulation were established by preparing PEG-based solid dispersion (SD) using hot melting method and then adding taste masking agents. The PEG 6000 was melted at 70℃ and then 4 mg drug was dispersed at different ratios (1:2, 1:3, 1:4, 1:8, 1:12), followed by cooling for 1 hour at a room temperature. The resulting SD powders were the milled and sieved. For further taste masking, SD and Eudragit EPO (1:0.5, 1:1, 1:2) were physically mixed. Then, content uniformity of the drug was determined by HPLC and in vitro taste masking efficiency was measured with an electronic tongue (E-Tongue). OND SR granules were manufactured by melt granulation method using lipophilic melt binders. The melt binder was melted at 80℃ and then 10 mg OND was added at different ratios (1:1, 1:2, 1:3), followed by cooling for 3 min at room temperature. The resulting products were passed through a 20-mesh sieve. In vitro dissolution rate of OND SR granules were investigated in the pH shifting condition for 24 hour. The compatibility study of OND and DEX was conducted at 40ºC/RH 75% for 14 days. After that, ODTs were prepared via direct compression after mixing DEX formulation, OND SR granule, various diluents, disintegrant and magnesium stearate (Mg-st). Changes in dissolution rate between before and after compression were checked by calculating f2 value and investigated in vitro disintegration time. The DEX formulation showed good content uniformity (Mean%: 96.9±1.08%, RSD: 1.11%) and good taste masking efficiency (distance to drug: 378±5.86). When the ratio of OND to Comptirol 888 ATO was 1: 3, OND SR granule was released below 50% for 2 hour in gastric condition and showed sustained release effect for 22 hour in intestinal condition. Compatibility of OND and DEX was good solid state compatibility in physical mixtures. The drug contents and physical appearance were almost unchanged during 14 days. When L-HPC was used as a cushioning agent, the change in drug release before and after compression was the smallest (f2=67.75) and the in vitro disintegration time for all formulations of ODT was between 22.17 and 304.83 s. As a result of Differential scanning calorimetry (DSC) and Powder X-ray diffraction (PXRD) measurements, the preparation process and presence of excipients in both of the two drug formulations did not interfere with the crystallinity of the drugs.-
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Graduate School of Ajou University > Department of Pharmacy > 3. Theses(Master)
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