"The book covers a wide range of topics and, as such, it will serve as a valuable reference for pharmaceutical scientists, toxicologists, academicians, and the graduate students." (Doody's, May 2009)
21 Kapitel, durchgesehen und aktualisiert: In diesem neu aufgelegten Standardwerk erkl ren Wirkstoffforscher aus dem akademischen und industriellen Umfeld alle Faktoren, die die Bioverf gbarkeit von Wirkstoffen beeinflussen. Teil 1 konzentriert sich auf die Messung physikalischer Eigenschaften (in vivo und in vitro), Teil 2 diskutiert L slichkeit und gastrointestinale Absorption, Teil 3 widmet sich Fragen des Metabolismus und der Exkretion. Der besonders intensiv berarbeitete Teil 4 geht auf moderne Computermodelle zur Absch tzung der Bioverf gbarkeit potenzieller Wirksubstanzen ein. Der letzte Teil besch ftigt sich mit der Verbesserung der Bioverf gbarkeit durch ma geschneiderte Syntheseprozesse. -- Mit Beitr gen von Wissenschaftlern f hrender Pharmaunternehmen wie Pfizer, AstraZeneca und Roche
List of Contributors.
Preface.
A Personal Foreword.
1 Introduction: The Why and How of Drug Bioavailability Research (Han van de Waterbeemd and Bernard Testa).
1.1 Defining Bioavailability.
1.2 Presentation and Layout of the Book.
Part One Physicochemical Aspects of Drug Dissolution and Solubility.
2 Aqueous Solubility in Drug Discovery Chemistry, DMPK, and Biological Assays (Nicola Colclough, Linette Ruston, and Kin Tam).
2.1 Introduction.
2.2 Aqueous Solubility in Hit Identification.
2.3 Aqueous Solubility in Lead Identification and Lead Optimization.
2.4 Conclusions.
3 Gastrointestinal Dissolution and Absorption of Class II Drugs (Arik S. Dahan and Gordon L. Amidon).
3.1 Introduction.
3.2 Drug Absorption and the BCS.
3.3 Class II Drugs.
3.4 GI Physiological Variables Affecting Class II Drug Dissolution.
3.5 In Vitro Dissolution Tests for Class II Drugs.
3.6 BCS-Based FDA Guidelines: Implications for Class II Drugs.
3.7 Conclusions.
4 In Silico Prediction of Solubility (Andrew M. Davis and Pierre Bruneau).
4.1 Introduction.
4.2 What Solubility Measures to Model?
4.3 Is the Data Set Suitable for Modeling?
4.4 Descriptors and Modeling Methods for Developing Solubility Models.
4.5 Comparing Literature Solubility Models.
4.6 What Is the Influence of the Domain of Applicability?
4.7 Can We Tell when Good Predictions Are Made?
4.8 Conclusions.
Part Two Physicochemical and Biological Studies of Membrane Permeability and Oral Absorption.
5 Physicochemical Approaches to Drug Absorption (Han van de Waterbeemd).
5.1 Introduction.
5.2 Physicochemical Properties and Pharmacokinetics.
5.3 Dissolution and Solubility.
5.4 Ionization (pKa).
5.5 Molecular Size and Shape.
5.6 Hydrogen Bonding.
5.7 Lipophilicity.
5.8 Permeability.
5.9 Amphiphilicity.
5.10 Drug-Like Properties.
5.11 Computation Versus Measurement of Physicochemical Properties.
5.12 Outlook.
6 High-Throughput Measurement of Physicochemical Properties (Barbara P. Mason).
6.1 Introduction.
6.2 Positioning of Physicochemical Screening in Drug Discovery.
6.3 "Fit for Purpose"Versus "Gold Standard".
6.4 Solubility.
6.5 Dissociation Constants, pKa.
6.6 Lipophilicity.
6.7 Permeability.
6.8 Data Interpretation, Presentation, and Storage.
6.9 Conclusions.
7 An Overview of Caco-2 and Alternatives for Prediction of Intestinal Drug Transport and Absorption (Anna-Lena Ungell and Per Artursson).
7.1 Introduction.
7.2 Cell Cultures for Assessment of Intestinal Permeability.
7.3 Correlation to Fraction of Oral Dose Absorbed.
7.4 Cell Culture and Transport Experiments.
7.5 Active Transport Studies in Caco-2 Cells.
7.6 Metabolism Studies using Caco-2 Cells.
7.7 Conclusions.
8 Use of Animals for the Determination of Absorption and Bioavailability (Chris Logan).
8.1 Introduction.
8.2 Consideration of Absorption and Bioavailability.
8.3 Choice of Animal Species.
8.4 Methods.
8.5 In Vivo Methods for Determining Bioavailability.
8.6 Inhalation.
8.7 Relevance of Animal Models.
8.8 Prediction of Dose in Man.
8.9 Conclusions.
9 In Vivo Permeability Studies in the Gastrointestinal Tract of Humans (Niclas Petri and Hans Lennernäs).
9.1 Introduction.
9.2 Definitions of Intestinal Absorption, Presystemic Metabolism, and Absolute Bioavailability.
9.3 Methodological Aspects of In Vitro Intestinal Perfusion Techniques.
9.4 Paracellular Passive Diffusion.
9.5 Transcellular Passive Diffusion.
9.6 Carrier-Mediated Intestinal Absorption.
9.7 Jejunal Transport and Metabolism.
9.8 Regional Differences in Transport and Metabolism of Drugs.
9.9 Conclusions.
Part Three Role of Transporters and Metabolism in Oral Absorption.
10 Transporters in the Gastrointestinal Tract (Pascale Anderle and Carsten U. Nielsen).
10.1 Introduction.
10.2 Active Transport Along the Intestine and Influence on Drug Absorption.
10.3 Transporters and Genomics.
10.4 Structural Requirements for Targeting Absorptive Intestinal Transporters.
10.5 Transporters and Diseased States of the Intestine.
10.6 Summary and Outlook.
11 Hepatic Transport (Kazuya Maeda, Hiroshi Suzuki, and Yuichi Sugiyama).
11.1 Introduction.
11.2 Hepatic Uptake.
11.3 Biliary Excretion.
11.4 Sinusoidal Efflux.
11.5 Prediction of Hepatobiliary Transport of Substrates from In Vitro Data.
11.6 Genetic Polymorphism of Transporters and Its Clinical Relevance.
11.7 Transporter-Mediated Drug–Drug Interactions.
11.8 Concluding Remarks.
12 The Importance of Gut Wall Metabolism in Determining Drug Bioavailability (Christopher Kohl).
12.1 Introduction.
12.2 Physiology of the Intestinal Mucosa.
12.3 Drug-Metabolizing Enzymes in the Human Mucosa.
12.4 Oral Bioavailability.
12.5 Clinical Relevance of Gut Wall First-Pass Metabolism.
13 Modified Cell Lines (Guangqing Xiao and Charles L. Crespi).
13.1 Introduction.
13.2 Cell/Vector Systems.
13.3 Expression of Individual Metabolic Enzymes.
13.4 Expression of Transporters.
13.5 Summary and Future Perspectives.
Part Four Computational Approaches to Drug Absorption and Bioavailability.
14 Calculated Molecular Properties and Multivariate Statistical Analysis (Ulf Norinder).
14.1 Introduction.
14.2 Calculated Molecular Descriptors.
14.3 Statistical Methods.
14.4 Applicability Domain.
14.5 Training and Test Set Selection and Model Validation.
14.6 Future Outlook.
15 Computational Absorption Prediction (Christel A.S. Bergström, Markus Haeberlein, and Ulf Norinder).
15.1 Introduction.
15.2 Descriptors Influencing Absorption.
15.3 Computational Models of Oral Absorption.
15.4 Software for Absorption Prediction.
15.5 Future Outlook.
16 In Silico Prediction of Human Bioavailability (David J. Livingstone and Han van de Waterbeemd).
16.1 Introduction.
16.2 Concepts of Pharmacokinetics and Role of Oral Bioavailability.
16.3 In Silico QSAR Models of Oral Bioavailability.
16.4 Prediction of the Components of Bioavailability.
16.5 Using Physiological Modeling to Predict Oral Bioavailability.
16.6 Conclusions.
17 Simulations of Absorption, Metabolism, and Bioavailability (Michael B. Bolger, Robert Fraczkiewicz, and Viera Lukacova).
17.1 Introduction.
17.2 Background.
17.3 Use of Rule-Based Computational Alerts in Early Discovery.
17.4 Mechanistic Simulation (ACAT Models) in Early Discovery.
17.5 Mechanistic Simulation of Bioavailability (Drug Development).
17.6 Regulatory Aspects of Modeling and Simulation (FDA Critical Path Initiative).
17.7 Conclusions.
18 Toward Understanding P-Glycoprotein Structure–Activity Relationships (Anna Seelig).
18.1 Introduction.
18.2 Measurement of P-gp Function.
18.3 Predictive In Silico Models.
18.4 Discussion.
Part Five Drug Development Issues.
19 Application of the Biopharmaceutics Classification System Now and in the Future (Bertil Abrahamsson and Hans Lennernäs).
19.1 Introduction.
19.2 Definition of Absorption and Bioavailability of Drugs Following Oral Administration.
19.3 Dissolution and Solubility.
19.4 The Effective Intestinal Permeability (Peff).
19.5 Luminal Degradation and Binding.
19.6 The Biopharmaceutics Classification System.
19.7 Conclusions.
20 Prodrugs (Bernard Testa).
20.1 Introduction.
20.2 Why Prodrugs?
20.3 How Prodrugs?
20.4 Conclusions.
21 Modern Delivery Strategies: Physiological Considerations for Orally Administered Medications (Clive G. Wilson and Werner Weitschies).
21.1 Introduction.
21.2 The Targets.
21.3 The Upper GI Tract: Mouth and Esophagus.
21.4 Mid-GI Tract: Stomach and Intestine.
21.5 The Lower GI Tract: The Colon.
21.6 Pathophysiological Effects on Transit.
21.7 Pathophysiological Effects on Permeability.
21.8 pH.
21.9 Conclusions.
22 Nanotechnology for Improved Drug Bioavailability (Marjo Yliperttula and Arto Urtti).
22.1 Introduction.
22.2 Nanotechnological Systems in Drug Delivery.
22.3 Delivery via Nanotechnologies.
22.4 Key Issues and Future Prospects.
Index.