蘭索拉唑微粒及奈米粒緩釋劑型之設計及評估

Milind Sadashiv Alai; 賴敏嵐

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/61752

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DC 欄位	值	語言
dc.contributor.advisor	林文貞教授(Prof. Wen-Jen Lin)
dc.contributor.author	Milind Sadashiv Alai	en
dc.contributor.author	賴敏嵐	zh_TW
dc.date.accessioned	2021-06-16T13:11:51Z	-
dc.date.available	2018-07-29
dc.date.copyright	2013-09-24
dc.date.issued	2013
dc.date.submitted	2013-07-30
dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/61752	-
dc.description.abstract	Lansoprazole (LPZ) is acid-labile and water insoluble drug used in the treatment of acid related disorders such as gastro-esophageal reflux disease (GERD). However, due to its short plasma half life, lansoprazole can not control a night-time (nocturnal) acidity especially in the case of GERD where the secretory activity of proton pump returns. My dissertation was aimed to develop sustained-release microparticles and nanoparticles to ameliorate the nocturnal acid breakthrough event while being administered on a once daily basis. In the first part of the study, LPZ loaded Eudragit RS100 microparticles were prepared using a solvent emulsion-evaporation method, and further enteric coated with HPMCP and Eudragit S100 by the spray drying method. The investigated enteric microparticles showed an excellent acid resistance. The rate of drug release was significantly delayed by an enteric-coated microparticles than a commercial extended release capsule (RICHR). The developed enteric-coated microparticles were capable of maintaining a constant plasma level of LPZ up to 24 h with a linear in vitro-in vivo correlation and promoted an ulcer healing activity in Wistar rats. In the second part of the study, LPZ loaded Eudragit RS100 nanoparticles (ERSNPs-LPZ) and PLGA nanoparticles (PLGANPs-LPZ) were formulated by solvent evaporation technique using probe sonication. The prepared nanoparticles showed sustained drug release up to 24 h. The LPZ transported across Caco-2 cell monolayers was significantly improved by positively charged nanoparticles (ERSNPs-LPZ) than negatively charged nanoparticles (PLGANPs-LPZ) while PLGANPs-LPZ improved LPZ transport in the presence of permeation enhancer. Similar results were observed with the fluorescent nanoparticles in the cellular uptake study. Confocal microscopic images of Caco-2 cell monolayers demonstrated nanoparticles localization in cytoplasm. The correlation between in vitro LPZ release and LPZ transported across Caco-2 cell monolayers suggested that drug absorption via nanoparticles was mainly controlled by drug release rate and extent of nanoparticles absorbed by Caco-2 cells. In vivo biodistribution study demonstrated that the total amount of positively charged fluorescent nanoparticles adhered to the ulcerated and non-ulcerated regions were higher than negatively charged fluorescent nanoparticles. Oral administration of non-enteric and enteric-coated capsule containing LPZ-loaded nanoparticles showed extended LPZ release up to 24 h which was linearly correlated to LPZ transported across a Caco-2 cell monolayer and promoted an ulcer healing activity in Wistar rats. There was no significant difference in the bioavailability of non-enteric and enteric coated nanoparticles formulations and nanoparticles showed higher bioavailability compared to enteric microparticles. Finally, non-enteric and enteric-coated capsules containing ERSNPs-LPZ were found to be the most efficacious formulations in the treatment of GERD especially to control nocturnal acid breakthrough.	en
dc.description.provenance	Made available in DSpace on 2021-06-16T13:11:51Z (GMT). No. of bitstreams: 1 ntu-102-D96423007-1.pdf: 8923866 bytes, checksum: 657392803496b3e6b050233caa6b2654 (MD5) Previous issue date: 2013	en
dc.description.tableofcontents	Abstract …………………………………………………………….………………………. I Table of contents …………………………………………………………………….......... IV List of Tables ………………………………………………………………….................. VIII List of Figures ……………………………………………………..............…….............… XI Schemes …………………………………………………………………......................... XVII Chapter 1: Introduction ……………………………………………........................…..….. 1 1.1 Gastro esophageal reflux disease (GERD) ………………..........................……...... 1 1.1.1 Background ……….......................….…........….........………….................. 1 1.1.2 Treatment of GERD ………………….......................….….................…..... 2 1.1.3 Hurdles and limitations of current PPI therapies in the management of GERD ………………………………………………………………….... 5 1.1.4 Emerging therapies for the management of GERD ….……………….…..... 5 1.2 Proton-pump inhibitors (PPI’s) 1.2.1 Properties of PPIs ……….………………………………….….……..…… 11 1.2.2 Pharmacology of PPIs ………….……………………………….……..….. 13 1.2.3 Employed ways of stable formulations of PPIs ……………….……..….... 18 1.3 Microparticles as drug delivery systems ………………………………………...... 21 1.3.1 Properties of microparticles ……………………………………………..... 21 1.3.2 Microencapsulation methods …………………………………………....... 23 1.3.3 Microparticles as controlled drug delivery devices ……………………..... 26 1.4 Nanoparticles as drug delivery systems ……………………………………..…..... 27 1.4.1 Preparation methods ……………………………………….……………... 28 1.4.2 Transport mechanisms of nanoparticles ….………………….………..….. 33 1.4.3 In vitro model for nanoparticles transport across intestinal epithelia …...... 38 1.4.4 Applications of nanoparticles in oral drug delivery …………………....… 39 1.4.5 Marketed formulation of nanoparticles ….………………….…………..... 39 1.5 Eudragit Polymers ……………………………………………………………....… 42 Chapter 2: Objective of study ………..............………………………..............………...… 46 Chapter 3: Materials and Equipments ……………………….…………………..….…... 47 3.1 Model compounds …………………..............……….……………….................... 47 3.1.1 Lansoprazole ………………..............……………....................................... 47 3.1.2 Coumarin 6 …………………..............…………………………….............. 48 3.2 Excipients …………………..............…………………………………………...... 49 3.2.1 EudragitR RS100 …………………..............……….……………................ 49 3.2.2 Poly (lactic-co-glycolic acid) ………………..............…………….............. 50 3.2.3 EudragitR S100 …………………..............…………………........................ 51 3.2.4 Hydroxy propyl methylcellulose phthalate (HPMCP) …………….............. 52 3.3 Chemicals and equipments ..……………..............……………………….............. 53 3.3.1 Formulation …………………..............…………….……………................. 53 3.3.2 In vitro release …………………..............…………….……………............. 55 3.3.3 Cell culture …………………..............…………….……………................. 56 3.3.4 Animals …………………..............…………….……………....................... 58 3.4 Buffers …………………..............…………………………………….................... 58 Chapter 4 : Experimental methods ……………………………………………………….. 60 4.1 Lansoprazole Delayed-Release Enteric Microparticles To Prevent The Nocturnal Acid Breakthrough In Case Of Gastro-Esophageal Reflux Disease: In Vitro And In Vivo Evaluation ……………………………………….……………………..… 60 4.1.1 Introduction ………………………………………………………………… 60 4.1.2 HPLC method Validation …………………..............…………………......... 61 4.1.3 Preparation of ERSMPs …………………..............…………………............ 62 4.1.4 Preparation of enteric coated microparticles and enteric coated capsule ....... 65 4.1.5 Characterization of ERSMPs, enteric microparticles and enteric coated capsules …………………………………..……………………………….... 67 4.1.6 Acid resistance study …………………..............……………….…….......... 68 4.1.7 Stability of LPZ in pH 7.4 …………..............……………..…………......... 69 4.1.8 In vitro drug release …………..............…………………............................. 69 4.1.9 In vivo animal study …………..............………………………………......... 70 4.2 Novel Non-Enteric Coated Lansoprazole Nanoparticles For Treatment of Gastroesophageal Reflux Disease: Preparation, In Vitro Characterization And In Vivo Evaluation ………………..……….…..………………………………….. 73 4.2.1 Introduction ………………………………………………………………… 73 4.2.2 HPLC and fluorescence spectrophotometer validation …………………..… 74 4.2.3 Preparation of sustained release LPZ-loaded nanoparticles …....................... 75 4.2.4 Characterization of nanoparticles ……………………..…………………..... 79 4.2.5 Preparation and characterization of enteric coated capsules ……………..… 81 4.2.6 In vitro drug release ……………………..………………………………..… 82 4.2.7 In vitro Transport study ……………………..…………………..……..….... 83 4.2.8 Coumarin-6-loaded fluorescent nanoparticles ………………….…….….…. 85 4.2.9 Pharmacokinetic study ……………………..…………………....…………. 89 4.2.10 Pharmacodyamic study ……………………..……………………..………. 94 Chapter 5 : RESULT AND DISCUSSION ……………………….…………………..…... 96 5.1 Lansoprazole Delayed-Release Enteric Microparticles To Prevent The Nocturnal Acid Breakthrough In Case Of Gastro-Esophageal Reflux Disease: In Vitro And In Vivo Evaluation ……………………………………………..…. 96 5.1.1 HPLC method Validation ……………………..……………………..…….. 96 5.1.2 Characterization ERSMPs ……………………..…………………….…… 109 5.1.3 Characterization of enteric-coated microparticles and capsules ……..…... 120 5.1.4 Acid-resistance evaluation ……………………..……………………..….. 124 5.1.5 Stability of LPZ at pH 7.4 ……………………..…………………........…. 127 5.1.6 In vitro release ……………………..……………………..……….……… 129 5.1.7 In vivo pharmacokinetic study ……………..………….…………..............132 5.1.8 Ulcer healing response ……………………..……………………….……. 140 5.1.9 Summary ………………………………………………………………….. 142 5.2 Novel Non-Enteric Coated Lansoprazole Nanoparticles For Treatment of Gastroesophageal Reflux Disease: Preparation, In Vitro Characterization And In Vivo Evaluation …………………..…………………………………….…...… 143 5.2.1 Method Validation ……………………..……………………..…….…..…. 143 5.2.2 FT-IR and DSC study ……………………..…………………………….… 154 5.2.3 Effect of formulation variables on the properties of LPZ loaded EudragitR RS100 nanoparticles ……………..……………………..……………..…... 158 5.2.4 Characterization of PLGANPs-LPZ ……………………..…………..……. 165 5.2.5 Characterization of enteric coated capsules ……………………….…….... 168 5.2.6 In vitro Drug release ……………………..…………..……………..…..…. 169 5.2.7 Transport study in Caco-2 cells ……………………..……………..…….... 179 5.2.8 Correlation of drug release and cellular drug transport ……………..…..… 183 5.2.9 Characterization of coumarin-6 loaded nanoparticles …………………..… 184 5.2.10 Cellular uptake of coumarin-6 loaded nanoparticles …………………...... 186 5.2.11 Nanoparticles transport mechanism ……………………………………... 192 5.2.12 Biodistribution study ……………………..……………………..……..… 193 5.2.13 Pharmacokinetic study ……………………..………………………….… 196 (a) Non-enteric coated nanoparticles ……………………..……..………... 196 (b) Enteric coated capsules filled with nanoparticles ………………….…. 197 5.2.14 Ulcer healing response study ……………………..…………………....... 223 (a) Non-enteric coated nanoparticles …………………….…..………...…. 223 (b) Enteric coated nanoparticles ……………………..………………..…... 228 5.2.15 Summary ………………..………………..…............................................. 235 Chapter 6 : Conclusions ……………………………………………………………….…. 239 Chapter 7 : Prospective …………………………………………………………….……. 240 Chapter 8 : References …………………………………………………………………... 242
dc.language.iso	en
dc.subject	微米粒子	zh_TW
dc.subject	胃食道逆流與消化性潰瘍	zh_TW
dc.subject	奈米粒子	zh_TW
dc.subject	緩釋劑型	zh_TW
dc.subject	蘭索拉唑	zh_TW
dc.subject	Lansoprazole	en
dc.subject	Microparticles	en
dc.subject	Nanoparticles	en
dc.subject	Sustained release	en
dc.subject	Gastro-esophageal reflux disease	en
dc.title	蘭索拉唑微粒及奈米粒緩釋劑型之設計及評估	zh_TW
dc.title	DESIGN AND EVALUATION OF SUSTAINED RELEASE LANSOPRAZOLE MICRO- AND NANOPARTICLES FOR TREATMENT OF GASTROESOPHAGEAL REFLUX DISEASE	en
dc.type	Thesis
dc.date.schoolyear	101-2
dc.description.degree	博士
dc.contributor.oralexamcommittee	江樵熹教授(Prof.Chiao-Hsi Chiang),葉明功教授(Prof. Ming-Kung Yeh),林滿玉教授(Prof. Maan-Yuh Lin),方嘉佑教授(Prof. Jia-You Fang)
dc.subject.keyword	蘭索拉唑,微米粒子,奈米粒子,緩釋劑型,胃食道逆流與消化性潰瘍,	zh_TW
dc.subject.keyword	Lansoprazole,Microparticles,Nanoparticles,Sustained release,Gastro-esophageal reflux disease,	en
dc.relation.page	263
dc.rights.note	有償授權
dc.date.accepted	2013-07-31
dc.contributor.author-college	醫學院	zh_TW
dc.contributor.author-dept	藥學研究所	zh_TW
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