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My supervisor, Professor John Michael Haigh, for giving me this opportunity to undertake my research study with him and for his guidance, encouragement and financial support. I would also like to thank his wife, Mrs Lil Haigh for the keen interest and trust she has in me.
IN VITRO RELEASE OF KETOPROFEN FROM PROPRIETARY AND EXTEMPORANEOUSLY MANUFACTURED GELS A Thesis Submitted to Rhodes University in Fulfilment of the Requirements for the Degree of MASTER OF SCIENCE (PHARMACY) by Ralph Nii Okai Tettey-Amlalo December 2005 Faculty of Pharmacy Rhodes University Grahamstown i ABSTRACT Ketoprofen is a potent non-steroidal anti-inflammatory drug which is used for the treatment of rheumatoid arthritis The oral administration of ketoprofen can cause gastric irritation and adverse renal effects Transdermal delivery of the drug can bypass gastrointestinal disturbances and provide relatively consistent drug concentrations at the site of administration The release of ketoprofen from proprietary gel products from three different countries was evaluated by comparing the in vitro release profiles Twenty extemporaneously prepared ketoprofen gel formulations using Carbopol® polymers were manufactured The effect of polymer, drug concentration, pH and solvent systems on the in vitro release of ketoprofen from these formulations were investigated The gels were evaluated for drug content and pH The release of the drug from all the formulations obeyed the Higuchi principle Two static FDA approved diffusion cells, namely the modified Franz diffusion cell and the European Pharmacopoeia diffusion cell, were compared by measuring the in vitro release rate of ketoprofen from all the gel formulations through a synthetic silicone membrane High-performance liquid chromatography and ultraviolet spectrophotometric analytical techniques were both used for the analysis of ketoprofen The validated methods were employed for the determination of ketoprofen in the sample solutions taken from the receptor fluid Two of the three proprietary products registered under the same manufacturing license exhibited similar results whereas the third product differed significantly Among the variables investigated, the vehicle pH and solvent composition were found have the most significant effect on the in vitro release of ketoprofen from Carbopol® polymers The different grades of Carbopol® polymers showed statistically significantly different release kinetics with respect to lag time When evaluating the proprietary products, both the modified Franz diffusion cell and the European Pharmacopoeia diffusion cell were deemed adequate although higher profiles were generally obtained from the European Pharmacopoeia diffusion cells ii Smoother diffusion profiles were obtained from samples analysed by high-performance liquid chromatography than by ultraviolet spectrophotometry in both diffusion cells Sample solutions taken from Franz diffusion cells and analysed by ultraviolet spectrophotometry also produced smooth diffusion profiles Erratic and higher diffusion profiles were observed with samples taken from the European Pharmacopoeia diffusion cell and analysed by ultraviolet spectrophotometry The choice of diffusion cells and analytical procedure in product development must be weighed against the relatively poor reproducibility as observed with the European Pharmacopoeia diffusion cell iii ACKNOWLEDGEMENT I would like to sincerely thank the following people: My supervisor, Professor John Michael Haigh, for giving me this opportunity to undertake my research study with him and for his guidance, encouragement and financial support I would also like to thank his wife, Mrs Lil Haigh for the keen interest and trust she has in me Mr Dave Morley, Mr Leon Purdon and Mr Tichaona Samkange for their advice, assistance and technical expertise in the laboratory and to Mrs Prudence Mzangwa for ensuring the tidiness of the laboratory The Dean and Head, Professor Isadore Kanfer and the staff of the Faculty of Pharmacy for the use of departmental facilities Professor Roger Verbeeck for giving me his book on Dermatological and Transdermal Formulations and GraphPad PRISM® statistical software My colleagues in the Faculty for their friendship and support Sigma-Aldrich (Atlasville, South Africa) for the donation of ketoprofen which was facilitated by Professor Rod Bryan Walker Aspen Pharmacare (Port Elizabeth, South Africa), Gattefossé (Saint-Priest, France), Noveon Inc (Cleveland, USA) for the donation of excipients My parents, especially my Father, who has always believed in me and taught me the true meaning of hard work Finally I would like to give thanks to the Almighty God for strength, determination and power to succeed no matter what storms or challenges life brings my way I would also like to thank him for the life of my son iv STUDY OBJECTIVES Ketoprofen is a non-steroidal anti-inflammatory, analgesic and antipyretic drug used for the treatment of rheumatoid osteoarthritis, ankylosing spondylitis and gout It is more potent than the other non-steroidal anti-inflammatory drugs (NSAIDs) with respect to some effects such as anti-inflammatory and analgesic activities Although ketoprofen is rapidly absorbed, metabolized and excreted, it causes some gastrointestinal complaints such as nausea, dyspepsia, diarrhoea, constipation and some renal side effects like other NSAIDs Therefore, there is a great interest in developing topical dosage forms of these NSAIDs to avoid the oral side effects and provide relatively consistent drug concentrations at the application site for prolonged periods The objectives of this study were: To develop and validate a suitable high-performance liquid chromatographic method for the determination of ketoprofen from topical gel formulations To develop and validate a suitable ultraviolet spectrophotometric method for the determination of ketoprofen from topical gel formulations To extemporaneously manufacture topical gel formulations using Carbopol® polymers and study the effect of polymer type, pH, loading concentration and solvent composition on the in vitro release of ketoprofen To compare and contrast the in vitro release rates of ketoprofen from proprietary gel products and extemporaneously prepared topical gel formulations using the Franz diffusion cell and the European Pharmacopoeia diffusion cell To compare and contrast the in vitro release rates of different proprietary gel products and extemporaneously prepared topical gel formulations using ultraviolet spectrophotometry and high-performance liquid chromatography utilizing both the Franz diffusion cell and the European Pharmacopoeia diffusion cell v TABLE OF CONTENTS ABSTRACT ii ACKNOWLEDGEMENT iv STUDY OBJECTIVES v TABLE OF CONTENTS vi LIST OF TABLES xii LIST OF FIGURES xiii CHAPTER ONE TRANSDERMAL DRUG DELIVERY 1.1 PAST PROGRESS, CURRENT STATUS AND FUTURE PROSPECTS OF TRANSDERMAL DRUG DELIVERY 1.1.1 1.1.2 1.1.3 1.1.4 1.2 Introduction Rationale for transdermal drug delivery Advantages and drawbacks of transdermal drug delivery Innovations in transdermal drug delivery PERCUTANEOUS ABSORPTION 1.2.1 1.2.2 1.2.2.1 1.2.2.2 1.2.2.3 1.2.2.4 1.2.3 1.2.3.1 1.2.3.2 1.2.3.3 1.2.4 1.2.5 1.2.5.1 1.2.5.1.1 1.2.5.2 1.2.5.2.1 1.2.5.2.2 1.2.5.2.3 1.2.5.2.4 1.2.5.2.5 1.2.5.2.6 1.2.5.2.7 Introduction Human skin Structure and functions of skin The epidermis The viable epidermis 10 The dermis .10 Routes of drug permeation across the skin 10 Transcellular pathway 11 Intercellular pathway .11 Appendageal pathway 12 Barrier function of the skin 13 Enhancing transdermal drug delivery 14 Chemical approach 14 Chemical penetration enhancers 16 Physical approach 17 Iontophoresis 17 Electroporation 19 Phonophoresis 20 Microneedle 22 Pressure waves .23 Other approaches 23 Synergistic effect of enhancers 24 vi 1.2.6 1.2.6.1 1.2.6.1.1 1.2.6.1.2 1.2.6.1.3 1.2.7 1.2.7.1 1.2.7.2 1.2.7.3 1.3 MATHEMATICAL PRINCIPLES IN TRANSMEMBRANE DIFFUSION 27 1.3.1 1.3.2 1.3.2.1 1.3.2.2 1.3.3 1.4 Selection of drug candidates for transdermal drug delivery 24 Biological properties of the drug .25 Potency .25 Half-life 25 Toxicity 25 Physicochemical properties of the drug 25 Oil-water partition co-efficient 25 Solubility and molecular dimensions .26 Polarity and charge 26 Introduction 27 Fickian model 27 Fick’s first law of diffusion 27 Fick’s second law of diffusion .28 Higuchi model 30 METHODS FOR STUDYING PERCUTANEOUS ABSORPTION 32 1.4.1 1.4.2 1.4.2.1 1.4.2.2 Introduction 32 Diffusion cell design 32 Franz and modified Franz diffusion cell 33 European Pharmacopoeia diffusion cell 34 CHAPTER TWO 36 KETOPROFEN MONOGRAPH 36 2.1 PHYSICOCHEMICAL PROPERTIES OF KETOPROFEN 36 2.1.1 2.1.2 2.1.3 2.1.4 2.1.5 2.1.6 2.1.7 2.1.8 2.1.9 2.1.10 2.1.11 2.1.12 2.1.13 2.1.14 Introduction 36 Description .36 Stereochemistry 37 Melting point 37 Solubility 37 Dissociation constant .38 Maximum flux 38 Partition co-efficient and permeability co-efficient .38 Optical rotation 38 Synthesis 39 Stability 42 Ultraviolet absorption 43 Infrared spectrum .43 Nuclear magnetic resonance spectrum 43 vii 2.2 CLINICAL PHARMACOLOGY OF KETOPROFEN 45 2.2.1 2.2.2 2.2.3 2.2.4 2.2.4.1 2.2.4.2 2.2.5 2.2.6 2.2.7 2.2.8 2.3 Anti-inflammatory effects 45 Analgesic and antipyretic effects .45 Mechanism of action 45 Therapeutic use 47 Indications 47 Contraindications .47 Adverse reactions 48 Toxicology .49 Drug interactions 50 Pharmaceutics 51 PHARMACOKINETICS OF TOPICAL KETOPROFEN 52 CHAPTER THREE 56 IN VITRO ANALYSIS OF KETOPROFEN 56 3.1 DEVELOPMENT AND VALIDATION OF AN HIGH-PERFORMANCE LIQUID CHROMATOGRAPHIC METHOD FOR THE DETERMINATION OF KETOPROFEN 56 3.1.1 3.1.1.1 3.1.1.2 3.1.1.2.1 3.1.1.2.2 3.1.1.2.3 3.1.1.2.4 3.1.1.2.5 3.1.1.2.6 3.1.1.2.7 3.1.1.3 3.1.1.3.1 3.1.1.3.2 3.1.1.3.3 3.1.1.4 3.1.1.5 3.1.2 3.1.2.1 3.1.2.2 3.1.2.3 3.1.2.3.1 3.1.2.3.2 3.1.2.3.3 3.1.2.4 3.1.2.5 Method development .56 Introduction 56 Experimental 57 Reagents .57 Instrumentation 57 Ultraviolet detection 59 Column selection 59 Mobile phase selection .61 Preparation of selected mobile phase 62 Preparation of stock solutions 63 Optimisation of the chromatographic conditions 63 Detector wavelength 63 Choice of column .63 Mobile phase composition 64 Chromatographic conditions 65 Conclusion .65 Method validation 66 Introduction 66 Accuracy and bias 66 Precision 67 Repeatability 67 Intermediate precision 68 Reproducibility 68 Specificity and selectivity 69 Limit of detection and limit of quantitation 69 viii 3.1.2.6 3.1.2.7 3.1.2.8 3.2 Linearity and range 70 Sample solution stability 71 Conclusion .72 DEVELOPMENT AND VALIDATION OF AN ULTRAVIOLET SPECTROPHOTOMETRIC METHOD FOR THE DETERMINATION OF KETOPROFEN 73 3.2.1 3.2.1.1 3.2.1.2 3.2.1.2.1 3.2.1.3 3.2.1.3.1 3.2.1.3.2 3.2.1.3.3 3.2.1.4 3.2.1.4.1 3.2.1.4.2 3.2.1.4.3 3.2.1.4.4 3.2.1.5 3.2.2 3.2.2.1 3.2.2.2 3.2.2.2.1 3.2.2.2.2 3.2.2.2.3 3.2.2.3 3.2.2.4 3.2.2.5 3.1.2.6 Method development .73 Introduction 73 Principles of ultraviolet-visible absorption spectroscopy 73 Beer-Lambert law 73 Experimental 76 Reagents .76 Instrumentation 76 Preparation of stock solutions 76 Optimization of spectrophotometric conditions .76 Solvent 76 Ultraviolet detection 77 Concentration of solute 77 Spectrophotometric conditions 77 Conclusion .77 Method validation 78 Accuracy and bias 78 Precision 78 Repeatability 78 Intermediate precision 78 Reproducibility 79 Limit of detection and limit of quantitation 79 Linearity and range 79 Sample solution stability 80 Conclusion .80 CHAPTER FOUR 81 THE IN VITRO RELEASE OF KETOPROFEN 81 4.1 IN VITRO DISSOLUTION METHODOLOGY 81 4.1.1 4.1.2 4.1.2.1 4.1.2.2 4.1.2.3 4.1.2.4 4.1.2.5 4.1.2.6 4.1.2.7 4.1.2.8 Introduction 81 In vitro release testing 82 Diffusion cell system .82 Synthetic membrane .83 Receptor medium .83 Sample applications 86 Number of samples 87 Sampling time 88 Sample analysis 88 Diffusion profile comparison 88 ix CHAPTER FIVE 90 FORMULATIONS OF PROPRIETARY AND EXTEMPORANEOUS TOPICAL KETOPROFEN GEL PREPARATIONS USING CARBOPOL® POLYMERS AND CO-POLYMERS 90 5.1 DERMATOLOGICAL FORMULATIONS 90 5.1.1 5.1.2 5.1.2.1 5.1.2.2 5.1.2.3 5.2 EXCIPIENTS 94 5.2.1 5.2.2 5.2.3 5.2.4 5.2.5 5.3 Proposed design .99 Preliminary studies 99 Preparation of extemporaneous topical gel formulations 99 Physical characterization of extemporaneous topical gel formulations .100 Drug content 100 pH 102 Viscosity 102 In vitro dissolution studies .102 DIFFUSION PROFILES AND RELEASE KINETIC DATA OF PROPRIETARY KETOPROFEN CONTAINING TOPICAL GEL PREPARATIONS FROM THREE COUNTRIES 103 5.4.1 5.4.2 5.4.2.1 5.4.2.2 5.4.2.3 5.4.3 5.4.4 5.5 Gelling agents 94 Triethanolamine .97 Propylene glycol 97 Ethanol .97 Transcutol® HP 97 EXPERIMENTAL 99 5.3.1 5.3.2 5.3.3 5.3.4 5.3.4.1 5.3.4.2 5.3.4.3 5.3.4.4 5.4 Introduction 90 Formulation of dermatological products 91 Ointments .91 Gels 92 Emulsions .93 Introduction 103 Results 104 Composition of proprietary products .104 Drug content and pH readings .105 In vitro release of ketoprofen .106 Discussion 108 Conclusion .110 DIFFUSION PROFILES AND RELEASE KINETIC DATA OF EXTEMPORANEOUS TOPICAL KETOPROFEN GEL PREPARATIONS USING CARBOPOL® POLYMERS AND CO-POLYMERS 111 5.5.1 5.5.2 Introduction 111 Results 112 x ... Effect of molarity and pH on the diffusion profile of ketoprofen .85 Effect of temperature on the diffusion profile of ketoprofen 86 Effect of mass on the diffusion profile of ketoprofen ... spectrum of ketoprofen 44 Nuclear magnetic resonance spectrum of ketoprofen 44 Metabolism of ketoprofen 55 Figure 3.1 Typical chromatogram of a standard solution of ketoprofen... the analysis of ketoprofen 58 The effect of mobile phase composition on the retention time of ketoprofen 62 Effect of wavelength on the relative percent peak area of ketoprofen 63