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Aggregation of therapeutic proteins [[electronic resource] /] / edited by Wei Wang, Christopher J. Roberts
| Aggregation of therapeutic proteins [[electronic resource] /] / edited by Wei Wang, Christopher J. Roberts |
| Pubbl/distr/stampa | Hoboken, NJ, : Wiley, c2010 |
| Descrizione fisica | 1 online resource (514 p.) |
| Disciplina | 615.5/8 |
| Altri autori (Persone) |
WangWei <1957 Mar. 10->
RobertsChristopher John <1972-> |
| Soggetto topico |
Protein drugs
Aggregation (Chemistry) |
| ISBN |
1-118-04358-8
1-282-70798-1 9786612707988 0-470-76982-3 0-470-76981-5 |
| Formato | Materiale a stampa  |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
AGGREGATION OF THERAPEUTIC PROTEINS; CONTENTS; PREFACE; CONTRIBUTORS; CHAPTER 1: Fundamental Structures and Behaviors of Proteins; CHAPTER 2: Protein Aggregation Pathways, Kinetics, and Thermodynamics; CHAPTER 3: Identification and Impact of Aggregation-Prone Regions in Proteins and Therapeutic Monoclonal Antibodies; CHAPTER 4: External Factors Affecting Protein Aggregation; CHAPTER 5: Experimental Detection and Characterization of Protein Aggregates; CHAPTER 6: Approaches to Control Protein Aggregation during Bulk Production
CHAPTER 7: Protein Aggregation and Particle Formation: Effects of Formulation, Interfaces, and Drug Product Manufacturing OperationsCHAPTER 8: Approaches to Managing Protein Aggregation in Product Development; CHAPTER 9: Case Studies Involving Protein Aggregation; CHAPTER 10: Aggregation and Immunogenicity of Therapeutic Proteins; CHAPTER 11: Regulatory Perspective on Aggregates as a Product Quality Attribute; INDEX; color plate |
| Record Nr. | UNINA-9910140832103321 |
| Hoboken, NJ, : Wiley, c2010 | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Aggregation of therapeutic proteins / / edited by Wei Wang, Christopher J. Roberts
| Aggregation of therapeutic proteins / / edited by Wei Wang, Christopher J. Roberts |
| Edizione | [1st ed.] |
| Pubbl/distr/stampa | Hoboken, NJ, : Wiley, c2010 |
| Descrizione fisica | 1 online resource (514 p.) |
| Disciplina | 615.5/8 |
| Altri autori (Persone) |
WangWei <1957 Mar. 10->
RobertsChristopher John <1972-> |
| Soggetto topico |
Protein drugs
Aggregation (Chemistry) |
| ISBN |
1-118-04358-8
1-282-70798-1 9786612707988 0-470-76982-3 0-470-76981-5 |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
AGGREGATION OF THERAPEUTIC PROTEINS; CONTENTS; PREFACE; CONTRIBUTORS; CHAPTER 1: Fundamental Structures and Behaviors of Proteins; CHAPTER 2: Protein Aggregation Pathways, Kinetics, and Thermodynamics; CHAPTER 3: Identification and Impact of Aggregation-Prone Regions in Proteins and Therapeutic Monoclonal Antibodies; CHAPTER 4: External Factors Affecting Protein Aggregation; CHAPTER 5: Experimental Detection and Characterization of Protein Aggregates; CHAPTER 6: Approaches to Control Protein Aggregation during Bulk Production
CHAPTER 7: Protein Aggregation and Particle Formation: Effects of Formulation, Interfaces, and Drug Product Manufacturing OperationsCHAPTER 8: Approaches to Managing Protein Aggregation in Product Development; CHAPTER 9: Case Studies Involving Protein Aggregation; CHAPTER 10: Aggregation and Immunogenicity of Therapeutic Proteins; CHAPTER 11: Regulatory Perspective on Aggregates as a Product Quality Attribute; INDEX; color plate |
| Record Nr. | UNINA-9910819845003321 |
| Hoboken, NJ, : Wiley, c2010 | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Antimicrobial peptides [[electronic resource] /] / [editors, Joan Marsh and Jamie A. Goode]
| Antimicrobial peptides [[electronic resource] /] / [editors, Joan Marsh and Jamie A. Goode] |
| Pubbl/distr/stampa | Chichester, England ; ; New York, : Wiley, 1994 |
| Descrizione fisica | 1 online resource (293 p.) |
| Disciplina |
574.29
615/.3 |
| Altri autori (Persone) |
MarshJoan
GoodeJamie |
| Collana | Ciba Foundation symposium |
| Soggetto topico |
Peptide antibiotics
Protein drugs Peptides - Therapeutic use Microbial peptides |
| Soggetto genere / forma | Electronic books. |
| ISBN |
1-282-45501-X
9786612455018 0-470-51465-5 0-470-51466-3 |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
ANTIMICROBIAL PEPTIDES; Chairman's opening remarks; Design and synthesis of antimicrobial peptides; Gene-encoded antibiotics made in bacteria; General discussion I; Biosynthesis of defensins and other antimicrobial peptides; Antimicrobial peptides from amphibian skin: an overview; Gene-encoded antimicrobial peptides from plants; Drosophila as a model system for antibacterial peptides; Function of antimicrobial proteins in insects; General discussion I I; Anti bacterial peptides in insect vectors of tropical parasitic disease
Structu re-f u nction relationships of tachyplesins and their analoguesBactericidal permeability-increasing protein in host defence against Gram- negative bacteria and endotoxin; General discussion I I I; Potential therapeutic applications of magainins and other antimicrobial agents of animal origin; Primitive vertebrate immunity: what is the evolutionary derivation of molecules that define the adaptive immune system?; Antimicrobial proteins with homology to serine proteases; Antimicrobial peptides as agents of mucosal immunity; Closing remarks; Index of contributors; Subject index |
| Record Nr. | UNINA-9910144560203321 |
| Chichester, England ; ; New York, : Wiley, 1994 | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Antimicrobial peptides / / [editors, Joan Marsh and Jamie A. Goode]
| Antimicrobial peptides / / [editors, Joan Marsh and Jamie A. Goode] |
| Pubbl/distr/stampa | Chichester, England ; ; New York, : Wiley, 1994 |
| Descrizione fisica | 1 online resource (293 p.) |
| Disciplina | 615/.3 |
| Altri autori (Persone) |
MarshJoan
GoodeJamie |
| Collana | Ciba Foundation symposium |
| Soggetto topico |
Peptide antibiotics
Protein drugs Peptides - Therapeutic use Microbial peptides |
| ISBN |
1-282-45501-X
9786612455018 0-470-51465-5 0-470-51466-3 |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
ANTIMICROBIAL PEPTIDES; Chairman's opening remarks; Design and synthesis of antimicrobial peptides; Gene-encoded antibiotics made in bacteria; General discussion I; Biosynthesis of defensins and other antimicrobial peptides; Antimicrobial peptides from amphibian skin: an overview; Gene-encoded antimicrobial peptides from plants; Drosophila as a model system for antibacterial peptides; Function of antimicrobial proteins in insects; General discussion I I; Anti bacterial peptides in insect vectors of tropical parasitic disease
Structu re-f u nction relationships of tachyplesins and their analoguesBactericidal permeability-increasing protein in host defence against Gram- negative bacteria and endotoxin; General discussion I I I; Potential therapeutic applications of magainins and other antimicrobial agents of animal origin; Primitive vertebrate immunity: what is the evolutionary derivation of molecules that define the adaptive immune system?; Antimicrobial proteins with homology to serine proteases; Antimicrobial peptides as agents of mucosal immunity; Closing remarks; Index of contributors; Subject index |
| Record Nr. | UNINA-9910876801403321 |
| Chichester, England ; ; New York, : Wiley, 1994 | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Coordination chemistry in protein cages [[electronic resource] ] : principles, design, and applications / / edited by Takafumi Ueno, Yoshihito Watanabe
| Coordination chemistry in protein cages [[electronic resource] ] : principles, design, and applications / / edited by Takafumi Ueno, Yoshihito Watanabe |
| Pubbl/distr/stampa | Hoboken, N.J., : Wiley, [2013] |
| Descrizione fisica | 1 online resource (421 p.) |
| Disciplina | 615.1/9 |
| Altri autori (Persone) |
UenoTakafumi <1971->
WatanabeYoshihito |
| Soggetto topico |
Protein drugs
Protein drugs - Physiological transport Carrier proteins |
| ISBN |
1-118-57184-3
1-118-57181-9 1-299-38760-8 1-118-57169-X |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto | pt. I. Coordination chemistry in native protein cages -- pt. II. Design of metalloprotein cages -- pt. III. Coordination chemistry of protein assembly cages -- pt. IV. Applications in biology -- pt. V. Applications in nanotechnology -- pt. VI. Coordination chemistry inspired by protein cages. |
| Record Nr. | UNINA-9910139041303321 |
| Hoboken, N.J., : Wiley, [2013] | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Coordination chemistry in protein cages : principles, design, and applications / / edited by Takafumi Ueno, Yoshihito Watanabe
| Coordination chemistry in protein cages : principles, design, and applications / / edited by Takafumi Ueno, Yoshihito Watanabe |
| Edizione | [1st ed.] |
| Pubbl/distr/stampa | Hoboken, N.J., : Wiley, [2013] |
| Descrizione fisica | 1 online resource (421 p.) |
| Disciplina | 615.1/9 |
| Altri autori (Persone) |
UenoTakafumi <1971->
WatanabeYoshihito |
| Soggetto topico |
Protein drugs
Protein drugs - Physiological transport Carrier proteins |
| ISBN |
1-118-57184-3
1-118-57181-9 1-299-38760-8 1-118-57169-X |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto | pt. I. Coordination chemistry in native protein cages -- pt. II. Design of metalloprotein cages -- pt. III. Coordination chemistry of protein assembly cages -- pt. IV. Applications in biology -- pt. V. Applications in nanotechnology -- pt. VI. Coordination chemistry inspired by protein cages. |
| Record Nr. | UNINA-9910810586203321 |
| Hoboken, N.J., : Wiley, [2013] | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme
| Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme |
| Autore | Behme Stefan |
| Edizione | [Third edition.] |
| Pubbl/distr/stampa | Berlin, Germany : , : John Wiley & Sons, , [2022] |
| Descrizione fisica | 1 online resource (497 pages) |
| Disciplina | 615.19 |
| Soggetto topico |
Pharmaceutical industry
Protein drugs |
| Soggetto genere / forma | Electronic books. |
| ISBN |
3-527-83380-3
3-527-83381-1 3-527-83379-X |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
Cover -- Title Page -- Copyright -- Contents -- Preface to Third Edition -- Preface to First Edition -- List of Abbreviations -- Part I Introduction -- Chapter 1 Biopharmaceutical Production: Value Creation, Product Types, and Biological Basics Introduction -- 1.1 Role of Production in Pharmaceutical Biotechnology -- 1.1.1 Relationship Between Production and Development -- 1.1.2 Relationship Between Production and Marketing -- 1.2 Product Groups -- 1.2.1 Vaccines -- 1.2.2 Pharmaceuticals from Blood and Organs -- 1.2.3 Recombinant Therapeutic Proteins -- 1.2.4 Cell and Gene Therapeutics -- 1.2.5 Antibiotics -- 1.3 Basics of Biology -- 1.3.1 Cells and Microorganisms -- 1.3.1.1 Structure and Types of Cells -- 1.3.1.2 Metabolism -- 1.3.1.3 Reproduction and Aging -- 1.3.1.4 Viruses and Bacteriophages -- 1.3.1.5 Protein Biosynthesis -- 1.3.2 The Four Molecular Building Blocks of Biochemistry -- 1.3.2.1 Proteins -- 1.3.2.2 Nucleic Acids -- 1.3.2.3 Polysaccharides -- 1.3.2.4 Lipids -- Part II Technology -- Chapter 2 Manufacturing Process -- 2.1 Role of the Manufacturing Process in Biotechnology -- 2.2 Process Schematic and Evaluation -- 2.2.1 Drug Substance Manufacturing -- 2.2.2 Drug Product Manufacturing -- 2.2.3 Key Factors for Process Evaluation -- 2.3 Cell Bank -- 2.3.1 Expression Systems -- 2.3.2 Microbial Systems -- 2.3.2.1 Mammalian Systems -- 2.3.2.2 Transgenic Systems -- 2.3.3 Manufacturing and Storage of the Cell Bank -- 2.4 Fermentation -- 2.4.1 Basic Principles -- 2.4.1.1 Cell Growth and Product Expression -- 2.4.1.2 Comparison of Batch and Continuous Processes -- 2.4.1.3 Sterility and Sterile Technology -- 2.4.1.4 Comparison of Fermentation with Mammalian Cells and Microorganisms -- 2.4.2 Technologies and Equipment -- 2.4.2.1 Fermentation in Suspension Culture -- 2.4.2.2 Adherent Cell Cultures -- 2.4.2.3 Transgenic Systems.
2.4.3 Raw Materials and Processing Aids -- 2.4.3.1 Nutrient Media -- 2.4.3.2 Water, Gases, and Other Processing Aids -- 2.4.4 Overview of Fermentation -- 2.5 Purification -- 2.5.1 Basic Principles -- 2.5.1.1 Basic Pattern of Purification -- 2.5.1.2 Types of Impurities -- 2.5.1.3 Principles of Separation Technologies -- 2.5.2 Technologies for Cell Separation and Product Isolation -- 2.5.2.1 Cell Separation -- 2.5.2.2 Cell Disruption, Solubilization, and Refolding -- 2.5.2.3 Concentration and Stabilization -- 2.5.3 Technologies for Final Purification -- 2.5.3.1 Chromatographic Processes -- 2.5.3.2 Precipitation and Extraction -- 2.5.3.3 Sterile Filtration and Virus Removal -- 2.5.4 Raw Materials and Processing Aids -- 2.5.4.1 Gels for Chromatography -- 2.5.4.2 Membranes for TFF -- 2.5.5 Overview of Purification -- 2.6 Formulation and Filling -- 2.6.1 Basic Principles -- 2.6.2 Freeze‐Drying -- 2.7 Labeling and Packaging -- Chapter 3 Analytics -- 3.1 Role of Analytics in Biotechnology -- 3.2 Product Analytics -- 3.2.1 Identity -- 3.2.2 Content -- 3.2.3 Purity -- 3.2.4 Activity -- 3.2.5 Appearance -- 3.2.6 Stability -- 3.2.7 Quality Criteria of Analytical Methods -- 3.2.8 Analytical Methods -- 3.2.8.1 Amino Acid Analysis -- 3.2.8.2 Protein Sequencing -- 3.2.8.3 Peptide Mapping -- 3.2.8.4 Protein Content -- 3.2.8.5 Electrophoresis -- 3.2.8.6 Western Blot -- 3.2.8.7 HCP Enzyme‐Linked Immunosorbent Assay (ELISA) -- 3.2.8.8 Analytical Chromatography -- 3.2.8.9 Infrared (IR) Spectroscopy -- 3.2.8.10 UV/Vis Spectroscopy -- 3.2.8.11 Mass Spectrometry -- 3.2.8.12 Glycoanalytics -- 3.2.8.13 PCR -- 3.2.8.14 DNA/RNA Sequencing -- 3.2.8.15 Endotoxins and Pyrogen Testing -- 3.2.8.16 Bioburden Test -- 3.2.8.17 Virus Testing -- 3.2.8.18 TEM -- 3.2.8.19 Circular Dichroism -- 3.2.8.20 Differential Scanning Calorimetry -- 3.3 Process Analytics -- 3.3.1 Fermentation. 3.3.2 Purification -- 3.3.3 Formulation and Packaging -- 3.4 Environmental Monitoring -- 3.5 Raw Material Testing -- 3.6 Product Comparability -- Part III Pharmacy -- Chapter 4 Pharmacology and Drug Safety -- 4.1 Action of Drugs in Humans -- 4.1.1 Pharmacokinetics -- 4.1.2 Pharmacodynamics -- 4.1.2.1 Principles of Phenomenological Effects -- 4.1.2.2 Parameters of Drug Effects -- 4.2 Routes and Forms of Administration -- 4.3 Drug Study -- 4.3.1 Pre‐Clinical Study -- 4.3.2 Clinical Study -- 4.3.2.1 Phases of Clinical Studies -- 4.3.2.2 Design and Conduct of Clinical Trials -- 4.4 Path of the Drug from the Manufacturer to Patients -- 4.5 Drug Safety -- 4.5.1 Causes and Classification of Side Effects -- 4.5.2 Methods for Supervising Drug Safety (Pharmacovigilance) -- 4.5.3 Measures upon Incidence of Adverse Reactions -- Part IV Quality Assurance -- Chapter 5 Fundamentals of Quality Assurance -- 5.1 Basic Principles -- 5.2 Benefit of Quality Assurance Activities -- 5.3 Quality Management According to ISO 9000 -- 5.3.1 Fields of Activity -- 5.4 Structure of Quality Management Systems -- 5.5 Quality Management System Components in the Pharmaceutical Area -- 5.5.1 Documentation -- 5.5.2 Failure Prevention and Correction -- 5.5.3 Responsibility of Management and Training of Personnel -- 5.5.4 Audits -- 5.5.5 External Suppliers -- 5.5.6 Contract Review -- 5.6 Quality Assurance in Development -- Chapter 6 Quality Assurance in Manufacturing -- 6.1 GMP -- 6.1.1 Personnel -- 6.1.2 Premises and Equipment -- 6.1.2.1 Measures to Avoid External Contamination -- 6.1.2.2 Measures to Avoid Cross‐Contamination and Product Confusion -- 6.1.3 Equipment Qualification -- 6.1.4 Process Validation -- 6.1.5 Computer Validation -- 6.1.6 Documentation -- 6.2 Operative Workflows under GMP Conditions -- 6.2.1 Product Release and Deviation Management. 6.2.2 Changes in the Manufacturing Process -- 6.3 Production of Investigational Drugs -- A Case Study Part IV: Warning Letters by FDA -- Part V Pharmaceutical Law -- Chapter 7 Pharmaceutical Law and Regulatory Authorities -- 7.1 Fields of Pharmaceutical Law -- 7.2 Bindingness of Regulations -- 7.3 Authorities, Institutions, and Their Regulations -- 7.3.1 FDA -- 7.3.2 EMA -- 7.3.3 German Authorities -- 7.3.4 Japanese Authorities -- 7.3.5 Authorities of Growth Markets -- 7.3.5.1 China: National Medical Products Administration (NMPA) -- 7.3.5.2 Brazilian Agência Nacional de Vigilância Sanitária (National Health Surveillance Agency, ANVISA) -- 7.3.6 Other Important Institutions -- 7.3.6.1 US Pharmacopoeia -- 7.3.6.2 ICH -- 7.3.6.3 ISO -- 7.3.6.4 WHO -- 7.3.6.5 PIC/S -- 7.3.6.6 ISPE -- 7.3.6.7 PDA -- 7.4 Official Enforcement of Regulations -- 7.5 Drug Approval -- B Case Study Part V: Clinical Trials for Protein Products -- B.1 Mabthera®/Rituxan® -- B.2 Enbrel® -- B.2.1 Adult Patients with Rheumatoid Arthritis -- B.3 Remicade® Infliximab -- B.3.1 Adult Rheumatoid Arthritis -- B.4 Humira® 40 mg -- B.5 Lucentis® -- B.5.1 Treatment of Wet AMD -- B.6 Zaltrap® -- Part VI Production Facilities -- Chapter 8 Facility Design -- 8.1 Basic Principles -- 8.2 GMP‐Compliant Plant Design -- 8.2.1 Production Flow Diagram -- 8.2.2 Conceptual Plant Layout -- 8.2.2.1 Is the Facility Fit for the Intended Purpose? -- 8.2.2.2 Is the Facility cGMP Compliant? -- 8.2.2.3 Is the Facility Flexible? -- 8.2.2.4 Can the Facility Be Expanded? -- 8.2.2.5 Is It Possible to Separate the Core Process from the Support Functions? -- 8.2.2.6 Is the Plant Capacity Optimized and Are Synergies with Existing Facilities Used? -- 8.2.3 GMP Flow Analysis -- 8.2.4 Zoning Concept -- 8.3 Basic Concepts for Production Plants -- 8.3.1 Single‐ and Multiproduct Plants. 8.3.2 Fractal and Integrated Configuration -- 8.3.3 Flexible and Fixed Piping -- 8.3.4 Steel Tanks and Disposable Equipment -- 8.4 Clean and Plant Utilities -- 8.4.1 Clean Utilities -- 8.4.1.1 Water -- 8.4.1.2 Clean Steam -- 8.4.1.3 Gases and Process Air -- 8.4.2 Plant Utilities -- 8.4.3 Waste Management -- 8.5 Equipment Cleaning -- 8.6 Clean Rooms -- 8.6.1 Separation of Zones by Clean Room Design -- 8.6.2 Finishing of Floors, Walls, and Ceilings -- 8.6.3 HVAC Installations -- 8.6.4 Qualification -- 8.7 Automation -- 8.8 QC Laboratories -- 8.9 Location Factors -- 8.9.1 Cost -- 8.9.2 Personnel -- 8.9.3 Permitting -- 8.9.4 Synergies with Existing Facilities or Units -- 8.9.5 Logistics -- 8.9.6 Know‐How and Intellectual Property Protection -- 8.9.7 Other Risks -- 8.9.8 Market Access -- 8.9.9 Language and Culture -- Chapter 9 Planning, Construction, and Commissioning of a Manufacturing Plant -- 9.1 Steps of the Engineering Project -- 9.1.1 Planning -- 9.1.2 Construction -- 9.1.3 Commissioning, Qualification, Validation -- 9.2 Project Schedules -- 9.3 Cost Estimates -- 9.4 Organization of an Engineering Project -- 9.4.1 Expert Groups Involved -- 9.4.2 Role and Selection of Contractors -- 9.4.3 Contracts and Scope Changes -- 9.5 Successful Execution of an Engineering Project -- 9.6 Legal Aspects of Facility Engineering -- 9.6.1 Health, Safety, and Environmental Law -- 9.6.2 Building Law -- Part VII Economy -- Chapter 10 Production Costs -- 10.1 Drug Life Cycle -- 10.2 Position of the Manufacturing Costs in the Overall Cost Framework -- 10.3 Basic Principles of Cost Calculation -- 10.3.1 Nominal Accounting - Actual Accounting -- 10.3.2 Cost Accounting - Profit and Loss Accounting -- 10.3.3 Direct Costs - Indirect Costs -- 10.3.4 Fixed Costs - Variable Costs -- 10.3.5 Relevant and Irrelevant Costs -- 10.3.6 Cost Type, Cost Center, and Cost Unit. 10.4 Costs of Biotechnological Manufacturing Processes. |
| Record Nr. | UNINA-9910555013503321 |
Behme Stefan
|
||
| Berlin, Germany : , : John Wiley & Sons, , [2022] | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme
| Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme |
| Autore | Behme Stefan |
| Edizione | [Third edition.] |
| Pubbl/distr/stampa | Berlin, Germany : , : John Wiley & Sons, , [2022] |
| Descrizione fisica | 1 online resource (497 pages) |
| Disciplina | 615.19 |
| Soggetto topico |
Pharmaceutical industry
Protein drugs |
| ISBN |
3-527-83380-3
3-527-83381-1 3-527-83379-X |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
Cover -- Title Page -- Copyright -- Contents -- Preface to Third Edition -- Preface to First Edition -- List of Abbreviations -- Part I Introduction -- Chapter 1 Biopharmaceutical Production: Value Creation, Product Types, and Biological Basics Introduction -- 1.1 Role of Production in Pharmaceutical Biotechnology -- 1.1.1 Relationship Between Production and Development -- 1.1.2 Relationship Between Production and Marketing -- 1.2 Product Groups -- 1.2.1 Vaccines -- 1.2.2 Pharmaceuticals from Blood and Organs -- 1.2.3 Recombinant Therapeutic Proteins -- 1.2.4 Cell and Gene Therapeutics -- 1.2.5 Antibiotics -- 1.3 Basics of Biology -- 1.3.1 Cells and Microorganisms -- 1.3.1.1 Structure and Types of Cells -- 1.3.1.2 Metabolism -- 1.3.1.3 Reproduction and Aging -- 1.3.1.4 Viruses and Bacteriophages -- 1.3.1.5 Protein Biosynthesis -- 1.3.2 The Four Molecular Building Blocks of Biochemistry -- 1.3.2.1 Proteins -- 1.3.2.2 Nucleic Acids -- 1.3.2.3 Polysaccharides -- 1.3.2.4 Lipids -- Part II Technology -- Chapter 2 Manufacturing Process -- 2.1 Role of the Manufacturing Process in Biotechnology -- 2.2 Process Schematic and Evaluation -- 2.2.1 Drug Substance Manufacturing -- 2.2.2 Drug Product Manufacturing -- 2.2.3 Key Factors for Process Evaluation -- 2.3 Cell Bank -- 2.3.1 Expression Systems -- 2.3.2 Microbial Systems -- 2.3.2.1 Mammalian Systems -- 2.3.2.2 Transgenic Systems -- 2.3.3 Manufacturing and Storage of the Cell Bank -- 2.4 Fermentation -- 2.4.1 Basic Principles -- 2.4.1.1 Cell Growth and Product Expression -- 2.4.1.2 Comparison of Batch and Continuous Processes -- 2.4.1.3 Sterility and Sterile Technology -- 2.4.1.4 Comparison of Fermentation with Mammalian Cells and Microorganisms -- 2.4.2 Technologies and Equipment -- 2.4.2.1 Fermentation in Suspension Culture -- 2.4.2.2 Adherent Cell Cultures -- 2.4.2.3 Transgenic Systems.
2.4.3 Raw Materials and Processing Aids -- 2.4.3.1 Nutrient Media -- 2.4.3.2 Water, Gases, and Other Processing Aids -- 2.4.4 Overview of Fermentation -- 2.5 Purification -- 2.5.1 Basic Principles -- 2.5.1.1 Basic Pattern of Purification -- 2.5.1.2 Types of Impurities -- 2.5.1.3 Principles of Separation Technologies -- 2.5.2 Technologies for Cell Separation and Product Isolation -- 2.5.2.1 Cell Separation -- 2.5.2.2 Cell Disruption, Solubilization, and Refolding -- 2.5.2.3 Concentration and Stabilization -- 2.5.3 Technologies for Final Purification -- 2.5.3.1 Chromatographic Processes -- 2.5.3.2 Precipitation and Extraction -- 2.5.3.3 Sterile Filtration and Virus Removal -- 2.5.4 Raw Materials and Processing Aids -- 2.5.4.1 Gels for Chromatography -- 2.5.4.2 Membranes for TFF -- 2.5.5 Overview of Purification -- 2.6 Formulation and Filling -- 2.6.1 Basic Principles -- 2.6.2 Freeze‐Drying -- 2.7 Labeling and Packaging -- Chapter 3 Analytics -- 3.1 Role of Analytics in Biotechnology -- 3.2 Product Analytics -- 3.2.1 Identity -- 3.2.2 Content -- 3.2.3 Purity -- 3.2.4 Activity -- 3.2.5 Appearance -- 3.2.6 Stability -- 3.2.7 Quality Criteria of Analytical Methods -- 3.2.8 Analytical Methods -- 3.2.8.1 Amino Acid Analysis -- 3.2.8.2 Protein Sequencing -- 3.2.8.3 Peptide Mapping -- 3.2.8.4 Protein Content -- 3.2.8.5 Electrophoresis -- 3.2.8.6 Western Blot -- 3.2.8.7 HCP Enzyme‐Linked Immunosorbent Assay (ELISA) -- 3.2.8.8 Analytical Chromatography -- 3.2.8.9 Infrared (IR) Spectroscopy -- 3.2.8.10 UV/Vis Spectroscopy -- 3.2.8.11 Mass Spectrometry -- 3.2.8.12 Glycoanalytics -- 3.2.8.13 PCR -- 3.2.8.14 DNA/RNA Sequencing -- 3.2.8.15 Endotoxins and Pyrogen Testing -- 3.2.8.16 Bioburden Test -- 3.2.8.17 Virus Testing -- 3.2.8.18 TEM -- 3.2.8.19 Circular Dichroism -- 3.2.8.20 Differential Scanning Calorimetry -- 3.3 Process Analytics -- 3.3.1 Fermentation. 3.3.2 Purification -- 3.3.3 Formulation and Packaging -- 3.4 Environmental Monitoring -- 3.5 Raw Material Testing -- 3.6 Product Comparability -- Part III Pharmacy -- Chapter 4 Pharmacology and Drug Safety -- 4.1 Action of Drugs in Humans -- 4.1.1 Pharmacokinetics -- 4.1.2 Pharmacodynamics -- 4.1.2.1 Principles of Phenomenological Effects -- 4.1.2.2 Parameters of Drug Effects -- 4.2 Routes and Forms of Administration -- 4.3 Drug Study -- 4.3.1 Pre‐Clinical Study -- 4.3.2 Clinical Study -- 4.3.2.1 Phases of Clinical Studies -- 4.3.2.2 Design and Conduct of Clinical Trials -- 4.4 Path of the Drug from the Manufacturer to Patients -- 4.5 Drug Safety -- 4.5.1 Causes and Classification of Side Effects -- 4.5.2 Methods for Supervising Drug Safety (Pharmacovigilance) -- 4.5.3 Measures upon Incidence of Adverse Reactions -- Part IV Quality Assurance -- Chapter 5 Fundamentals of Quality Assurance -- 5.1 Basic Principles -- 5.2 Benefit of Quality Assurance Activities -- 5.3 Quality Management According to ISO 9000 -- 5.3.1 Fields of Activity -- 5.4 Structure of Quality Management Systems -- 5.5 Quality Management System Components in the Pharmaceutical Area -- 5.5.1 Documentation -- 5.5.2 Failure Prevention and Correction -- 5.5.3 Responsibility of Management and Training of Personnel -- 5.5.4 Audits -- 5.5.5 External Suppliers -- 5.5.6 Contract Review -- 5.6 Quality Assurance in Development -- Chapter 6 Quality Assurance in Manufacturing -- 6.1 GMP -- 6.1.1 Personnel -- 6.1.2 Premises and Equipment -- 6.1.2.1 Measures to Avoid External Contamination -- 6.1.2.2 Measures to Avoid Cross‐Contamination and Product Confusion -- 6.1.3 Equipment Qualification -- 6.1.4 Process Validation -- 6.1.5 Computer Validation -- 6.1.6 Documentation -- 6.2 Operative Workflows under GMP Conditions -- 6.2.1 Product Release and Deviation Management. 6.2.2 Changes in the Manufacturing Process -- 6.3 Production of Investigational Drugs -- A Case Study Part IV: Warning Letters by FDA -- Part V Pharmaceutical Law -- Chapter 7 Pharmaceutical Law and Regulatory Authorities -- 7.1 Fields of Pharmaceutical Law -- 7.2 Bindingness of Regulations -- 7.3 Authorities, Institutions, and Their Regulations -- 7.3.1 FDA -- 7.3.2 EMA -- 7.3.3 German Authorities -- 7.3.4 Japanese Authorities -- 7.3.5 Authorities of Growth Markets -- 7.3.5.1 China: National Medical Products Administration (NMPA) -- 7.3.5.2 Brazilian Agência Nacional de Vigilância Sanitária (National Health Surveillance Agency, ANVISA) -- 7.3.6 Other Important Institutions -- 7.3.6.1 US Pharmacopoeia -- 7.3.6.2 ICH -- 7.3.6.3 ISO -- 7.3.6.4 WHO -- 7.3.6.5 PIC/S -- 7.3.6.6 ISPE -- 7.3.6.7 PDA -- 7.4 Official Enforcement of Regulations -- 7.5 Drug Approval -- B Case Study Part V: Clinical Trials for Protein Products -- B.1 Mabthera®/Rituxan® -- B.2 Enbrel® -- B.2.1 Adult Patients with Rheumatoid Arthritis -- B.3 Remicade® Infliximab -- B.3.1 Adult Rheumatoid Arthritis -- B.4 Humira® 40 mg -- B.5 Lucentis® -- B.5.1 Treatment of Wet AMD -- B.6 Zaltrap® -- Part VI Production Facilities -- Chapter 8 Facility Design -- 8.1 Basic Principles -- 8.2 GMP‐Compliant Plant Design -- 8.2.1 Production Flow Diagram -- 8.2.2 Conceptual Plant Layout -- 8.2.2.1 Is the Facility Fit for the Intended Purpose? -- 8.2.2.2 Is the Facility cGMP Compliant? -- 8.2.2.3 Is the Facility Flexible? -- 8.2.2.4 Can the Facility Be Expanded? -- 8.2.2.5 Is It Possible to Separate the Core Process from the Support Functions? -- 8.2.2.6 Is the Plant Capacity Optimized and Are Synergies with Existing Facilities Used? -- 8.2.3 GMP Flow Analysis -- 8.2.4 Zoning Concept -- 8.3 Basic Concepts for Production Plants -- 8.3.1 Single‐ and Multiproduct Plants. 8.3.2 Fractal and Integrated Configuration -- 8.3.3 Flexible and Fixed Piping -- 8.3.4 Steel Tanks and Disposable Equipment -- 8.4 Clean and Plant Utilities -- 8.4.1 Clean Utilities -- 8.4.1.1 Water -- 8.4.1.2 Clean Steam -- 8.4.1.3 Gases and Process Air -- 8.4.2 Plant Utilities -- 8.4.3 Waste Management -- 8.5 Equipment Cleaning -- 8.6 Clean Rooms -- 8.6.1 Separation of Zones by Clean Room Design -- 8.6.2 Finishing of Floors, Walls, and Ceilings -- 8.6.3 HVAC Installations -- 8.6.4 Qualification -- 8.7 Automation -- 8.8 QC Laboratories -- 8.9 Location Factors -- 8.9.1 Cost -- 8.9.2 Personnel -- 8.9.3 Permitting -- 8.9.4 Synergies with Existing Facilities or Units -- 8.9.5 Logistics -- 8.9.6 Know‐How and Intellectual Property Protection -- 8.9.7 Other Risks -- 8.9.8 Market Access -- 8.9.9 Language and Culture -- Chapter 9 Planning, Construction, and Commissioning of a Manufacturing Plant -- 9.1 Steps of the Engineering Project -- 9.1.1 Planning -- 9.1.2 Construction -- 9.1.3 Commissioning, Qualification, Validation -- 9.2 Project Schedules -- 9.3 Cost Estimates -- 9.4 Organization of an Engineering Project -- 9.4.1 Expert Groups Involved -- 9.4.2 Role and Selection of Contractors -- 9.4.3 Contracts and Scope Changes -- 9.5 Successful Execution of an Engineering Project -- 9.6 Legal Aspects of Facility Engineering -- 9.6.1 Health, Safety, and Environmental Law -- 9.6.2 Building Law -- Part VII Economy -- Chapter 10 Production Costs -- 10.1 Drug Life Cycle -- 10.2 Position of the Manufacturing Costs in the Overall Cost Framework -- 10.3 Basic Principles of Cost Calculation -- 10.3.1 Nominal Accounting - Actual Accounting -- 10.3.2 Cost Accounting - Profit and Loss Accounting -- 10.3.3 Direct Costs - Indirect Costs -- 10.3.4 Fixed Costs - Variable Costs -- 10.3.5 Relevant and Irrelevant Costs -- 10.3.6 Cost Type, Cost Center, and Cost Unit. 10.4 Costs of Biotechnological Manufacturing Processes. |
| Record Nr. | UNINA-9910830723403321 |
|
Behme Stefan
|
||
| Berlin, Germany : , : John Wiley & Sons, , [2022] | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme
| Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme |
| Autore | Behme Stefan |
| Edizione | [Second, revised and expanded edition.] |
| Pubbl/distr/stampa | Weinheim, Germany : , : Wiley-VCH, , 2015 |
| Descrizione fisica | 1 online resource (458 p.) |
| Disciplina | 615.19 |
| Soggetto topico |
Pharmaceutical industry
Protein drugs |
| ISBN |
3-527-68308-9
3-527-68310-0 3-527-68309-7 |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
Cover; Contents; Preface; Preface to First Edition; List of Abbreviations; Part I: Introduction; Chapter 1 Biopharmaceutical Production: Value Creation, Product Types, and Biological Basics Introduction; 1.1 Role of Production in Pharmaceutical Biotechnology; 1.1.1 Relationship Between Production and Development; 1.1.2 Relationship Between Production and Marketing; 1.2 Product Groups; 1.2.1 Vaccines; 1.2.2 Pharmaceuticals from Blood and Organs; 1.2.3 Recombinant Therapeutic Proteins; 1.2.4 Cell and Gene Therapeutics; 1.2.5 Antibiotics; 1.3 Basics of Biology; 1.3.1 Cells and Microorganisms
1.3.1.1 Structure and Types of Cells1.3.1.2 Metabolism; 1.3.1.3 Reproduction and Aging; 1.3.1.4 Viruses and Bacteriophages; 1.3.1.5 Protein Biosynthesis; 1.3.2 The Four Molecular Building Blocks of Biochemistry; 1.3.2.1 Proteins; 1.3.2.2 Nucleic Acids; 1.3.2.3 Polysaccharides; 1.3.2.4 Lipids; Part II: Technology; Chapter 2 Manufacturing Process; 2.1 Role of the Manufacturing Process in Biotechnology; 2.2 Process Schematic and Evaluation; 2.2.1 Drug Substance Manufacturing; 2.2.2 Drug Product Manufacturing; 2.2.3 Key Factors for Process Evaluation; 2.3 Cell Bank; 2.3.1 Expression Systems 2.3.2 Microbial Systems2.3.2.1 Mammalian Systems; 2.3.2.2 Transgenic Systems; 2.3.3 Manufacturing and Storage of the Cell Bank; 2.4 Fermentation; 2.4.1 Basic Principles; 2.4.1.1 Cell Growth and Product Expression; 2.4.1.2 Comparison of Batch and Continuous Processes; 2.4.1.3 Sterility and Sterile Technology; 2.4.1.4 Comparison of Fermentation with Mammalian Cells and Microorganisms; 2.4.2 Technologies and Equipment; 2.4.2.1 Fermentation in Suspension Culture; 2.4.2.2 Adherent Cell Cultures; 2.4.2.3 Transgenic Systems; 2.4.3 Raw Materials and Processing Aids; 2.4.3.1 Nutrient Media 2.4.3.2 Water, Gases, and Other Processing Aids2.4.4 Overview of Fermentation; 2.5 Purification; 2.5.1 Basic Principles; 2.5.1.1 Basic Pattern of Purification; 2.5.1.2 Types of Impurities; 2.5.1.3 Principles of Separation Technologies; 2.5.2 Technologies for Cell Separation and Product Isolation; 2.5.2.1 Cell Separation; 2.5.2.2 Cell Disruption, Solubilization, and Refolding; 2.5.2.3 Concentration and Stabilization; 2.5.3 Technologies for Final Purification; 2.5.3.1 Chromatographic Processes; 2.5.3.2 Precipitation and Extraction; 2.5.3.3 Sterile Filtration and Virus Removal 2.5.4 Raw Materials and Processing Aids2.5.4.1 Gels for Chromatography; 2.5.4.2 Membranes for TFF; 2.5.5 Overview of Purification; 2.6 Formulation and Filling; 2.6.1 Basic Principles; 2.6.2 Freeze-Drying; 2.7 Labeling and Packaging; Chapter 3 Analytics; 3.1 Role of Analytics in Biotechnology; 3.2 Product Analytics; 3.2.1 Identity; 3.2.2 Content; 3.2.3 Purity; 3.2.4 Activity; 3.2.5 Appearance; 3.2.6 Stability; 3.2.7 Quality Criteria of Analytical Methods; 3.2.8 Analytical Methods; 3.2.8.1 Amino Acid Analysis; 3.2.8.2 Protein Sequencing; 3.2.8.3 Peptide Mapping; 3.2.8.4 Protein Content 3.2.8.5 Electrophoresis |
| Record Nr. | UNINA-9910787345403321 |
|
Behme Stefan
|
||
| Weinheim, Germany : , : Wiley-VCH, , 2015 | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme
| Manufacturing of pharmaceutical proteins : from technology to economy / / Stefan Behme |
| Autore | Behme Stefan |
| Edizione | [Second, revised and expanded edition.] |
| Pubbl/distr/stampa | Weinheim, Germany : , : Wiley-VCH, , 2015 |
| Descrizione fisica | 1 online resource (458 p.) |
| Disciplina | 615.19 |
| Soggetto topico |
Pharmaceutical industry
Protein drugs |
| ISBN |
3-527-68308-9
3-527-68310-0 3-527-68309-7 |
| Formato | Materiale a stampa |
| Livello bibliografico | Monografia |
| Lingua di pubblicazione | eng |
| Nota di contenuto |
Cover; Contents; Preface; Preface to First Edition; List of Abbreviations; Part I: Introduction; Chapter 1 Biopharmaceutical Production: Value Creation, Product Types, and Biological Basics Introduction; 1.1 Role of Production in Pharmaceutical Biotechnology; 1.1.1 Relationship Between Production and Development; 1.1.2 Relationship Between Production and Marketing; 1.2 Product Groups; 1.2.1 Vaccines; 1.2.2 Pharmaceuticals from Blood and Organs; 1.2.3 Recombinant Therapeutic Proteins; 1.2.4 Cell and Gene Therapeutics; 1.2.5 Antibiotics; 1.3 Basics of Biology; 1.3.1 Cells and Microorganisms
1.3.1.1 Structure and Types of Cells1.3.1.2 Metabolism; 1.3.1.3 Reproduction and Aging; 1.3.1.4 Viruses and Bacteriophages; 1.3.1.5 Protein Biosynthesis; 1.3.2 The Four Molecular Building Blocks of Biochemistry; 1.3.2.1 Proteins; 1.3.2.2 Nucleic Acids; 1.3.2.3 Polysaccharides; 1.3.2.4 Lipids; Part II: Technology; Chapter 2 Manufacturing Process; 2.1 Role of the Manufacturing Process in Biotechnology; 2.2 Process Schematic and Evaluation; 2.2.1 Drug Substance Manufacturing; 2.2.2 Drug Product Manufacturing; 2.2.3 Key Factors for Process Evaluation; 2.3 Cell Bank; 2.3.1 Expression Systems 2.3.2 Microbial Systems2.3.2.1 Mammalian Systems; 2.3.2.2 Transgenic Systems; 2.3.3 Manufacturing and Storage of the Cell Bank; 2.4 Fermentation; 2.4.1 Basic Principles; 2.4.1.1 Cell Growth and Product Expression; 2.4.1.2 Comparison of Batch and Continuous Processes; 2.4.1.3 Sterility and Sterile Technology; 2.4.1.4 Comparison of Fermentation with Mammalian Cells and Microorganisms; 2.4.2 Technologies and Equipment; 2.4.2.1 Fermentation in Suspension Culture; 2.4.2.2 Adherent Cell Cultures; 2.4.2.3 Transgenic Systems; 2.4.3 Raw Materials and Processing Aids; 2.4.3.1 Nutrient Media 2.4.3.2 Water, Gases, and Other Processing Aids2.4.4 Overview of Fermentation; 2.5 Purification; 2.5.1 Basic Principles; 2.5.1.1 Basic Pattern of Purification; 2.5.1.2 Types of Impurities; 2.5.1.3 Principles of Separation Technologies; 2.5.2 Technologies for Cell Separation and Product Isolation; 2.5.2.1 Cell Separation; 2.5.2.2 Cell Disruption, Solubilization, and Refolding; 2.5.2.3 Concentration and Stabilization; 2.5.3 Technologies for Final Purification; 2.5.3.1 Chromatographic Processes; 2.5.3.2 Precipitation and Extraction; 2.5.3.3 Sterile Filtration and Virus Removal 2.5.4 Raw Materials and Processing Aids2.5.4.1 Gels for Chromatography; 2.5.4.2 Membranes for TFF; 2.5.5 Overview of Purification; 2.6 Formulation and Filling; 2.6.1 Basic Principles; 2.6.2 Freeze-Drying; 2.7 Labeling and Packaging; Chapter 3 Analytics; 3.1 Role of Analytics in Biotechnology; 3.2 Product Analytics; 3.2.1 Identity; 3.2.2 Content; 3.2.3 Purity; 3.2.4 Activity; 3.2.5 Appearance; 3.2.6 Stability; 3.2.7 Quality Criteria of Analytical Methods; 3.2.8 Analytical Methods; 3.2.8.1 Amino Acid Analysis; 3.2.8.2 Protein Sequencing; 3.2.8.3 Peptide Mapping; 3.2.8.4 Protein Content 3.2.8.5 Electrophoresis |
| Record Nr. | UNINA-9910828171603321 |
|
Behme Stefan
|
||
| Weinheim, Germany : , : Wiley-VCH, , 2015 | ||
| Materiale a stampa | ||
| Lo trovi qui: Univ. Federico II | ||
| ||
