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دانلود کتاب Analytical Testing for the Pharmaceutical GMP Laboratory
دانلود کتاب آزمایش تحلیلی برای آزمایشگاه GMP دارویی
مشخصات کتاب
Analytical Testing for the Pharmaceutical GMP Laboratory
ویرایش:
نویسندگان: Kim Huynh-Ba
سری:
ISBN (شابک) : 1119120918, 9781119120919
ناشر: Wiley
سال نشر: 2022
تعداد صفحات: 417
[419]
زبان: English
فرمت فایل : PDF (درصورت درخواست کاربر به PDF، EPUB یا AZW3 تبدیل می شود)
حجم فایل: 6 Mb
قیمت کتاب (تومان) : 43,000
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توجه داشته باشید کتاب آزمایش تحلیلی برای آزمایشگاه GMP دارویی نسخه زبان اصلی می باشد و کتاب ترجمه شده به فارسی نمی باشد. وبسایت اینترنشنال لایبرری ارائه دهنده کتاب های زبان اصلی می باشد و هیچ گونه کتاب ترجمه شده یا نوشته شده به فارسی را ارائه نمی دهد.
توضیحاتی در مورد کتاب آزمایش تحلیلی برای آزمایشگاه GMP دارویی
راهنمای عملی در مورد تجزیه و تحلیل دارویی، نوشته شده توسط کارشناسان برجسته با تجربه صنعت گسترده ارائه می دهد
تست تحلیلی برای آزمایشگاه GMP دارویی ارائه می کند مروری کامل بر مقررات دارویی، فرآیندهای کاری، و بهترین شیوه های توسعه دارو که برای حفظ کیفیت و یکپارچگی داروها استفاده می شود. این کتاب با تمرکز بر مواد و محصولات دارویی با وزن مولکولی کوچکتر، دانش لازم را برای ایجاد آزمایشگاه دارویی برای پشتیبانی از سیستمهای کیفیت و در عین حال حفظ انطباق با مقررات شیوههای تولید خوب (GMP) فراهم میکند.
فصل های مختصر و در عین حال جامع شامل پوشش به روز مقررات دارو، روش های تجزیه و تحلیل دارویی، استراتژی های کنترل، توسعه آزمایش و اعتبار سنجی، انتقال روش، اسناد الکترونیکی داده ها و موارد دیگر است. هر فصل شامل فهرست مطالب، تعاریف کلمات اختصاری، فهرست مرجع و جداول و شکل های فراوان است. این منبع معتبر با توجه به فعالیتهای اصلی و چالشهای نظارتی آزمایشهای تحلیلی در توسعه و ساخت محصولات دارویی دارویی:
- ساختار، نقشها، دستورالعملهای اصلی و مقررات GMP FDA و ICH.
- تکنولوژیهای تحلیلی رایج مورد استفاده در آزمایشگاههای داروسازی را پوشش میدهد، از جمله نمونههایی از تکنیکهای تحلیلی مورد استفاده برای آزمایش آزادسازی و پایداری داروها.
- استراتژیهای کنترلی را که از سیستمهای کیفیتی که توسط مطالعات موردی در دنیای واقعی پشتیبانی میشوند، بررسی میکند.</ span>
- استفاده از آزمایش انحلال را برای محصولاتی مانند کپسولهای با رهش طولانی، آئروسلها و استنشاقها توضیح میدهد.
- درباره اسناد و شیوه های گزارش دهی خوب، برنامه های پایداری، و سیستم مدیریت اطلاعات آزمایشگاهی (LIMS) برای حفظ انطباق بحث می کند.
- شامل محاسبات، مثالهای کاربردی، و تصاویر برای کمک به خوانندگان در عملیات روزانه آزمایشگاهی است.
- حاوی اطلاعات کاربردی و الگوهایی برای ساختار داخلی است. فرآیندها یا رویههای عملیاتی استاندارد رایج (SOP).
آزمایش تحلیلی برای آزمایشگاه GMP دارویی یک امر ضروری است. دارای مرجعی برای دانشمندان داروسازی اولیه و با تجربه، شیمیدانان تحلیلی، داروسازان و متخصصان کنترل کیفیت. همچنین منبعی برای برنامههای آموزشی آزمایشگاهی GMP و یک کتاب درسی عالی برای دورههای کارشناسی و کارشناسی ارشد شیمی تجزیه در علوم دارویی یا برنامههای انطباق با مقررات است.
توضیحاتی درمورد کتاب به خارجی
Provides practical guidance on pharmaceutical analysis, written by leading experts with extensive industry experience
Analytical Testing for the Pharmaceutical GMP Laboratory presents a thorough overview of the pharmaceutical regulations, working processes, and drug development best practices used to maintain the quality and integrity of medicines. With a focus on smaller molecular weight drug substances and products, the book provides the knowledge necessary for establishing the pharmaceutical laboratory to support Quality Systems while maintaining compliance with Good Manufacturing Practices (GMP) regulations.
Concise yet comprehensive chapters contain up-to-date coverage of drug regulations, pharmaceutical analysis methodologies, control strategies, testing development and validation, method transfer, electronic data documentation, and more. Each chapter includes a table of contents, definitions of acronyms, a reference list, and ample tables and figures. Addressing the principal activities and regulatory challenges of analytical testing in the development and manufacturing of pharmaceutical drug products, this authoritative resource:
- Describes the structure, roles, core guidelines, and GMP regulations of the FDA and ICH.
- Covers the common analytical technologies used in pharmaceutical laboratories, including examples of analytical techniques used for the release and stability testing of drugs.
- Examines control strategies established from quality systems supported by real-world case studies.
- Explains the use of dissolution testing for products such as extended-release capsules, aerosols, and inhalers.
- Discusses good documentation and data reporting practices, stability programs, and the Laboratory Information Management System (LIMS) to maintain compliance.
- Includes calculations, application examples, and illustrations to assist readers in day-to-day laboratory operations.
- Contains practical information and templates to structure internal processes or common Standard Operating Procedures (SOPs).
Analytical Testing for the Pharmaceutical GMP Laboratory is a must-have reference for both early-career and experienced pharmaceutical scientists, analytical chemists, pharmacists, and quality control professionals. It is also both a resource for GMP laboratory training programs and an excellent textbook for undergraduate and graduate courses of analytical chemistry in pharmaceutical sciences or regulatory compliance programs.
فهرست مطالب
Cover Title Page Copyright Page Contents Einstein Quotation Preface About the Editor Biographies of Contributing Authors Editorial Notes Acknowledgments Chapter 1 Drug Regulations and the Pharmaceutical Laboratories 1.1 Introduction 1.2 Food and Drug Administration: Roles and Its Regulations 1.2.1 Code of Federation Regulations 1.2.2 FDA Guidance Documents 1.2.3 FDA Manual of Policies and Procedures 1.3 International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH) and Its Role 1.3.1 ICH Background 1.3.2 ICH Structure 1.3.3 ICH Organization 1.3.4 ICH Topics 1.4 Pharmaceutical Analysis 1.4.1 Analytical Testing 1.4.2 Interaction of the Analytical Development Department and Other Functional Areas 1.4.3 Drug Development Process 1.5 Summary List of Abbreviations References Chapter 2 Good Manufacturing Practices (GMPs) and the Quality Systems 2.1 Introduction to Good Manufacturing Practices 2.2 Objectives of GMPs 2.2.1 Definitions 2.2.2 Organization of 21 CFR Regulations 2.3 Personnel Qualification and Responsibilities – Subpart B 2.3.1 Responsibilities of the Quality Control Unit 2.3.2 Personnel Qualifications and Responsibilities 2.4 Equipment – Subpart D 2.4.1 Metrology Functions 2.4.2 Qualification Phases 2.5 Laboratory Controls 2.5.1 General Requirements 2.5.2 Testing and Release for Distribution 2.5.3 Stability Program 2.5.4 Retention Program 2.6 Records and Reports 2.7 Pharmaceutical Quality 2.7.1 Quality Manual 2.7.2 Quality Risk Management 2.7.3 Product Quality Review 2.7.4 Pharmaceutical Quality Systems List of Abbreviations References Chapter 3 Analytical Techniques Used in the GMP Laboratory 3.1 Introduction 3.2 Definitions 3.2.1 Raw Data and Analytical Data 3.2.2 Analyses 3.2.3 Analytical Documents 3.3 Basic Laboratory Procedures 3.3.1 Balances 3.3.2 Volumetric Glassware 3.3.3 Potentiometry (Ion-Selective Electrode) and pH Test 3.3.4 The Density Test 3.3.5 The Friability Test 3.3.6 The Hardness Test 3.3.7 The Titration Test 3.3.8 The Karl Fischer Titration–Water Determination 3.3.9 Loss on Drying 3.3.10 Residue on Ignition/Sulfated Ash 3.3.11 Thermo Gravimetric Analysis 3.3.12 Differential Scanning Calorimetry 3.3.13 The Disintegration Test 3.3.14 Particulate Matter 3.3.15 Osmolality 3.4 Chromatography 3.4.1 High-Performance Liquid Chromatography 3.4.2 Ultra-High-Pressure Liquid Chromatography 3.4.3 Detectors of Liquid Chromatography 3.4.4 System Suitability Tests for Chromatographic Methods 3.4.5 Maintenance of HPLC and UHPLC 3.4.6 Gas Chromatography 3.4.7 Thin-Layer Chromatography 3.4.8 Bio-Pharmaceutical Separations 3.5 Spectroscopic Sciences 3.5.1 Ultraviolet–Visible 3.5.2 Infrared-Absorption 3.5.3 Mass Spectroscopy 3.5.4 Atomic Absorption, Inductively Coupled Plasma, Inductively Coupled Plasma/Mass Spectrometry, and Inductively Coupled Plasma/Optical Emission Spectrometry 3.5.5 Nuclear Magnetic Resonance Spectroscopy 3.5.6 X-ray Absorption and X-ray Emission Spectrometry 3.6 Uniformity of Dosage Units 3.6.1 Weight Variation 3.6.2 Acceptance Criteria per USP <905> 3.7 Elemental Analysis 3.8 Appearance 3.9 Visual Inspection 3.10 Microbiological Testing 3.10.1 Microbial Limits 3.10.2 Sterility 3.10.3 Bacterial Endotoxins 3.10.4 Antimicrobial Effectiveness Testing 3.11 Summary References Chapter 4 Control Strategies for Pharmaceutical Development 4.1 Introduction 4.2 Quality-by-Design Concept 4.3 Risk Management 4.3.1 Risk Assessment 4.3.2 Risk Control 4.4 Establishing Specifications 4.4.1 What Is the Specification? 4.4.2 Typical Tests Included in the Specification of a Small Molecule Drug 4.4.3 Typical Tests Included in the Specification of Biological Drugs 4.4.4 Considerations of Setting Acceptance Criteria 4.5 Design of Experiments 4.5.1 Common Terms 4.5.2 Conducting the Study 4.5.3 Results Interpretation 4.5.4 Summary 4.6 Common Statistical Analysis 4.6.1 Mean, Standard Deviation (SD), and Relative Standard Deviation (RSD) 4.6.2 Confidence Interval 4.6.3 Statistical Significance (t-Test) 4.6.4 Outlier Detection 4.7 Summary List of Abbreviations References Chapter 5 Development and Validation of Analytical Procedures 5.1 Introduction 5.2 Method Development 5.2.1 Development of Physical, Chemical, and Microbiological Procedures 5.3 Qualification, Validation, and Verification 5.3.1 Qualification 5.3.2 Validation 5.3.3 Verification 5.3.4 Frequency of Study 5.4 Validation Parameters 5.4.1 Accuracy 5.4.2 Precision 5.4.3 Specificity 5.4.4 Quantitation and Detection Limits (QL and DL) 5.4.5 Linearity 5.4.6 Range 5.4.7 Robustness 5.4.8 System Suitability Tests (SST) 5.4.9 Stability of Samples During Analysis 5.4.10 Tie the Pieces Together 5.5 Validation for Physical, Chemical, Biotechnological, and Microbiological Procedures 5.6 Validation of In-process, Environmental, Release, and Stability Procedures 5.6.1 In-process Procedures 5.6.2 Environmental Procedures 5.6.3 Release and Stability Procedures 5.7 Other Procedures 5.7.1 Process Analytical Technology (PAT) 5.7.2 Parametric Release and Real-time Release 5.8 Validation of Procedures in Continuous and Batch Manufacturing 5.9 Summary List of Abbreviations References Chapter 6 Transfer of Analytical Procedures 6.1 Introduction 6.2 Purpose of Method Transfer 6.3 Transfer Options 6.3.1 Method Transfer Plan 6.3.2 Comparative Testing 6.3.3 Co-validation 6.3.4 Extended Validation or Partial Validation 6.3.5 Transfer Waiver 6.4 Method Transfer Process 6.4.1 Preparation Phase 6.4.2 Gap Analysis 6.4.3 Method Training Phase 6.4.4 Method Qualification Phase 6.5 Transfer Protocol 6.5.1 Content of a Transfer Protocol 6.5.2 Objectives/Scope 6.5.3 Roles and Responsibilities 6.5.4 Assessment of Receiving Lab 6.5.5 Materials, Facilities, and Instrumentation 6.5.6 Analyst Training 6.5.7 Qualification Procedure 6.5.8 Acceptance Criteria 6.5.9 Protocol Amendment and Deviation 6.6 Method Transfer Report 6.6.1 Objectives 6.6.2 Data Evaluation 6.6.3 Conclusion of Transfer Report 6.6.4 Analytical Transfer File 6.7 Related Documents 6.8 Handling Transfer Failures 6.9 Transfer to a Contract Lab 6.10 Transfer to an International Site 6.11 Summary References Chapter 7 Dissolution Testing in the Pharmaceutical Laboratory 7.1 Introduction 7.2 Regulatory and Compendial Role in Dissolution Testing 7.3 Theory 7.4 Equipment Operation and Sources of Error 7.4.1 Equipment Variables 7.4.2 Media Deaeration 7.4.3 Vibration 7.4.4 Water Bath of Dissolution Equipment 7.4.5 Glass Vessels 7.5 Common Errors of Dissolution Apparatus 7.5.1 USP Apparatus 1 and 2 7.5.2 USP Apparatus 3 7.5.3 USP Apparatus 4 7.5.4 USP Apparatus 5 7.5.5 USP Apparatus 6 7.5.6 USP Apparatus 7 7.6 Dissolution Method Considerations 7.6.1 Sample Introduction 7.6.2 Media Attributes 7.6.3 Observations 7.6.4 Sinkers 7.6.5 Filters 7.6.6 Manual Sampling 7.6.7 Automation of Dissolution Sampling 7.6.8 Cleaning of Dissolution Equipment 7.7 Method Development 7.7.1 Drug Properties 7.7.2 Dosage Form Properties 7.7.3 Dissolution Profile 7.7.4 Dissolution Media 7.7.5 Medium Volume 7.7.6 Deaeration 7.7.7 Speed 7.7.8 Sinkers 7.7.9 Filtration 7.7.10 Time Points – Immediate Release 7.7.11 Fast Stir or Infinity Point 7.7.12 Time Points for Extended-Release Products 7.8 Poorly Soluble Drugs 7.8.1 Sink Conditions 7.8.2 Apparatus Selection 7.8.3 The Discriminatory Power of the Method 7.9 Setting Specifications 7.10 Harmonization 7.11 Method Validation 7.12 Validation of Product Performance Parameters 7.12.1 Accuracy/Recovery 7.12.2 Selectivity 7.12.3 Solution Stability 7.12.4 Filter 7.12.5 Robustness 7.12.6 Intermediate Precision 7.12.7 Automated Methodology 7.13 Validation of the Analytical Finish 7.14 Method Transfer Considerations 7.14.1 Robustness 7.14.2 Details of the Analytical Method 7.14.3 Other Considerations 7.15 Good Manufacturing Practices (GMP) in the Dissolution Testing Laboratory 7.15.1 Metrology 7.15.2 Notebook Documentation 7.15.3 Equipment Qualification, Validation, and Method Critical Factors 7.15.4 Good Manufacturing Practice Audits 7.15.5 Training 7.16 Summary Acknowledgment List of Abbreviations Chapter 8 Analytical Data and the Documentation System 8.1 Introduction 8.1.1 Types of Documents 8.2 GMP for Records and Reports–Subpart J 8.2.1 General Requirements 8.2.2 Equipment Cleaning and Use Log 8.2.3 Component, Drug Product Container, Closure, and Labeling Records 8.2.4 Master Production and Control Records 8.2.5 Batch Production and Control Records 8.2.6 Production Record Review 8.2.7 Laboratory Records 8.3 Keeping Good Records 8.3.1 Writing Good Procedures 8.3.2 Following Procedures 8.4 Raw Data Documentation 8.4.1 Data Recording Practices 8.4.2 Witness Responsibilities 8.4.3 Changes in Notebook 8.4.4 Recording Date and Time 8.4.5 Voiding and Restoring GMP Records 8.4.6 Computer-Collected Data 8.4.7 Reporting Analytical Results 8.5 Samples, Reagents, Standards, Reference Standards 8.5.1 Samples 8.5.2 Reagents 8.5.3 Analytical Standards 8.5.4 Reference Standards 8.6 Drug Substance Analysis 8.7 Drug Product Analysis 8.8 Batch Release 8.8.1 Batch Packaging Record 8.8.2 Batch Processing Record 8.8.3 Distribution Record 8.9 Establishment of Specifications 8.9.1 Content of Specifications 8.9.2 Setting Specifications 8.9.3 Periodic Revisions 8.9.4 Test Procedures 8.10 Out-of-Specification (OOS) Results 8.10.1 Lab-Phase Investigation 8.10.2 Full Scale Investigation 8.11 Compendial Testing 8.11.1 Validation and Verification of Compendial Procedures 8.11.2 USP Reference Standards 8.12 Standard Operating Procedures 8.12.1 Control of SOPs 8.12.2 Format of SOPs 8.12.3 Flow of Documents 8.13 Analytical Documents 8.13.1 Hierarchy of Documentation Systems 8.13.2 Analytical Protocols 8.13.3 Analytical Reports 8.13.4 Annual Product Review 8.13.5 Changes to Documentation 8.14 Quality Assurance 8.14.1 Six Quality Systems and Their Supporting Programs 8.14.2 Quality System Performance 8.14.3 Lifecycle Management Approach for Analytical Procedures 8.14.4 Audit and Inspection program of the Laboratory 8.15 Summary References Chapter 9 Stability Program Supporting Pharmaceutical Products 9.1 Introduction 9.2 Regulatory Requirements for Stability Testing 9.3 Types of Stability Studies 9.3.1 Stability Studies of Materials Used in Clinical Development 9.3.2 Stability Studies of an Active Pharmaceutical Ingredient (API) or Drug Substance (DS) 9.3.3 Stability Studies to Support Formulation Development 9.3.4 Stability Studies to Support Drug Product (DP) Registration 9.3.5 Stability Studies to Support Marketed Products 9.3.6 Bulk Stability 9.3.7 In-Process Testing 9.3.8 In-Use Testing 9.3.9 Stability Studies to Support Excursions 9.4 Stability Program 9.4.1 Fundamental Principle of Stability 9.4.2 Specifications 9.5 Stability Chambers 9.6 Stability Sample Management 9.6.1 Study Start Date 9.6.2 Sample Pull Dates 9.6.3 Study End Date 9.6.4 Sample Inventory 9.7 Stability Protocol 9.7.1 Deviation of Stability Protocol 9.7.2 Study Cancelation 9.7.3 Reduce Testing with Bracketing and Matrixing 9.8 Stability Report 9.9 Annual Product Review (APR) 9.10 Summary List of Abbreviations References Chapter 10 Laboratory Information Management System (LIMS) and Electronic Data 10.1 Introduction 10.2 Analytical and Quality Data Management 10.3 Quality System 10.4 Process Control in Quality Management 10.5 Material Management 10.6 Product Release 10.7 Stability Studies 10.8 Cleaning Validation – Contamination Control 10.9 Equipment Management (Metrology) 10.10 Laboratory Operations 10.11 Automation of Risk Management 10.12 Automated Training Management 10.13 SOPs and Document Management 10.14 Audit Management and Compliance 10.15 Corrective and Preventive Actions (CAPAs) 10.16 Change Management 10.17 Computer Systems Validation 10.18 Evolution in the Data Integrity Regulation 10.19 Data Integrity 10.20 Quality Data 10.21 Benefits of Computerized Systems 10.22 Big Data List of Abbreviations References Index EULA
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