Wiley.com
Print this page Share

Prodrugs and Targeted Delivery: Towards Better ADME Properties

Jarkko Rautio (Editor), Raimund Mannhold (Series Editor), Hugo Kubinyi (Series Editor), Gerd Folkers (Series Editor)
ISBN: 978-3-527-32603-7
Hardcover
520 pages
January 2011
List Price: US $205.00
Government Price: US $138.19
Enter Quantity:   Buy
Prodrugs and Targeted Delivery: Towards Better ADME Properties (3527326030) cover image

Preface

PART ONE: Prodrug Design and Intellectual Property

PRODRUG STRATEGIES IN DRUG DESIGN
Prodrug Concept
Basics of Prodrug Design
Rationale for Prodrug Design
History of Prodrug Design
Recently Marketed Prodrugs
Concluding Remarks

THE MOLECULAR DESIGN OF PRODRUGS BY FUNCTIONAL GROUP
Introduction
The Prodrug Concept and Basics of Design
Common Functional Group Approaches in Prodrug Design
Conclusions

INTELLECTUAL PROPERTY PRIMER ON PHRAMACEUTICAL PATENTS WITH A SPECIAL EMPHASIS ON PRODRUGS AND METABOLITES
Introduction
Patents and FDA Approval Process
Obtaining a Patent
Conclusion

PART TWO: Prodrugs Addressing ADMET Issues

INCREADING LIPOPHILICITY FOR ORAL DRUG DELIVERY
Introduction
pKa, Degree of Ionization, Partition Coefficient, and Distribution Coefficient
Prodrug Strategies to Enhance Lipid Solubility
Prodrug Examples for Antibiotics
Antiviral Related Prodrugs
Cardiovascular Related Prodrugs
Lipophilic Prodrugs of Benzamidine Drugs
Miscellaneous Examples
Summary and Conclusion

MODULATING SOLUBILITY THROUGH PRODRUGS FOR ORAL AND IV DRUG DELIVERY
Introduction
Basics of Solubility and Oral/IV Drug Delivery
Prodrug Applications for Enhanced Aqueous Solubility
Challenges with Solubilizing Prodrugs of Insoluble Drugs
Additional Applications of Prodrugs for Modulating Solubility
Parallel Exploration of Analogues and Prodrugs in Drug Discovery (Commentary)
Conclusions

PRODRUGS DESIGNED TO TARGET TRANSPORTERS FOR ORAL DRUG DELIVERY
Introduction
Serendipity: An Actively Transported Prodrug
Requirements for Actively Transported Prodrugs
Peptide Transporters: PEPT1 and PEPT2
Monocarboxylate Transporters
Bile Acid Transporters
Conclusions

TOPICAL AND TRANSDERMAL DELIVERY USING PRODRUGS: MECHANISM OF ENHANCEMENT
Introduction
Arrangement of Water in the Stratum Corneum
A New Model for Diffusion Through the Stratum Corneum: The Biphasic Solubility Model
Equations for Quantifying Effects of Solubility on Diffusion Through the Stratum Corneum
Design of Prodrugs for Topical and Transdermal Delivery Based on the Biphasic Solubility Model
Comparison of Human and Mouse Skin Experiments
Summary

OCULAR DELIVERY USING PRODRUGS
Introduction
Criteria for an Ideal Ophthalmic Prodrug
Anatomy and Physiology of the Eye
Barriers to Ocular Drug Delivery
Influx and Efflux Transporters on the Eye
Transporter-Targeted Prodrug Approach
Drug Disposition in Ocular Delivery
Effect of Physiochemical Factors on Drug Disposition in Eye
Prodrug Strategy to Improve Ocular Bioavailability (Nontransporter-Targeted Approach)
Recent Patents and Marketed Ocular Prodrugs
Novel Formulation Approaches for Sustained Delivery of Prodrugs
Conclusion

REDUCING PRESYSTEMIC DRUG METABOLISM
Introduction
Presystemic Metabolic Barriers
Prodrug Approaches to Reduce Presystemic Drug Metabolism
Targeting Colon
Targeting Lymphatic Route
Conclusion

ENZYME-ACTIVATED PRODRUG STRATEGIES FOR SITE-SELECTIVE DRUG DELIVERY
Introduction
General Requirements for Enzyme-Activated Targeted Prodrug Strategy
Examples of Targeted Prodrug Strategies
Summary

PRODRUG APPROACHES FOR CENTRAL NERVOUS SYSTEM DELIVERY
Blood-Brain Barrier in CNS Drug Development
Prodrug Strategies
Prodrug Strategies Based Upon BBB Nutrient Transporters
Prodrug Strategies Based Upon BBB Receptors
CNS Prodrug Summary

DIRECTED ENZYME PRODRUG THERAPIES
Introduction
Theoretical Background of DEPT
Comparison of ADEPT and GDEPT
Enzymes in ADEPT and GDEPT
Design of Prodrugs
Strategies Used for the Improvement of DEPT Systems
Biological Data for ADEPT and GDEPT
Conclusions

PART THREE: Codrugs and Soft Drugs

IMPROVING THE USE OF DRUG COMBINATIONS THROUGH THE CODRUG APPROACH
Codrugs and Codrug Strategy
Ideal Codrug Characteristics
Examples of Marketed Codrugs
Topical Codrug Therapy for the Treatment of Ophthalmic Diseases
Codrugs for Transdermal Delivery
Codrugs of L-DOPA for the Treatment of Parkinson's Disease
Analgesic Codrugs Containing Nonsteroidal Anti-Inflammatory Agents
Analgesic Codrugs of Opioids and Cannabinoids
Codrugs Containing Anti-HIV Drugs

SOFT DRUGS
Introduction
Indications
Design Considerations
Case Study: The Discovery of Esmolol
Summary

PART FOUR: Preclinical and Clinical Considerations for Prodrugs

PHARMACOKINETIC AND BIOPHARMACEUTICAL CONSIDERATIONS IN PRODRUG DISCOVERY AND DEVELOPMENT
Introduction
Understanding Pharmacokinetic/Pharmacodynamic Relationships
Pharmacokinetics
Tools for the Prodrug Scientist
Enzymes Involved with Prodrug Conversion
Use of the Caco-2 System for Permeability and Active Transport Evaluation
XP13512: Improving PK Performance by Targeting Active Transport
Prodrug Absorption: Transport/Metabolic Conversion Interplay
Preabsorptive Degradation
Biopharmaceutical-Based PK Modeling for Prodrug Design
Conclusions

THE IMPACT OF PHARMACOGENETICS ON THE CLINICAL OUTCOMES OF PRODRUGS
Introduction
Clopidogrel and CYP2C19
Codeine and CYP2D6
Tamoxifen and CYP2D6
Fluorouracil Prodrugs and Carboxylesterase
Irinotecan and Carboxylesterase 2
Others
Drug Development Implication
Conclusions






Back to Top