Static and Dynamic Properties of Liquids: Proceedings of the International Symposium, Dubrovnik, Yugoslavia, June 27-July 2, 1988

Author:   Ronald Borchardt ,  Edward Kerns ,  Michael Hageman
Publisher:   Springer
Volume:   40
ISBN:  

9780387513843


Pages:   225
Publication Date:   01 January 1989
Format:   Undefined
Availability:   Out of stock   Availability explained


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Static and Dynamic Properties of Liquids: Proceedings of the International Symposium, Dubrovnik, Yugoslavia, June 27-July 2, 1988


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Overview

Traditionally, incorporating optimal drug-like properties into a structural lead was not considered by medicinal chemists to be their responsibility. Instead, medicinal chemists felt that the undesirable drug-like properties in their drug candidates would be fixed by preclinical development scientists. However, that view has changed in the past 5b 10 years, resulting in another significant paradigm shift in drug discovery. The most significant aspect of this latest paradigm shift is the recognition by medicinal chemists that the drug-like properties of structural hits, structural leads, and drug candidates are intrinsic properties of the molecules and that it is the responsibility of the medicinal chemist to optimize not only the pharmacological properties but also the drug-like properties of these molecules. Therefore, assessment of these drug-like properties is now done early in the drug discovery process on structural hits and structural leads as well as the design of screening libraries. Optimization of these drug-like properties is done through an iterative process in close collaboration with preclinical development scientists. This process is analogous to the process used by the medicinal chemist to characterize and optimize the pharmacological activity of their structural hits, leads and drug candidates.Recognizing these changes in the paradigm by which drugs are discovered, the American Association of Pharmaceutical Scientists (AAPS) has recently organized and sponsored two focused workshops in the area of profiling drug-like properties during drug discovery. The first workshop, entitled Pharmaceutical Profiling in Drug Discovery for Lead Selection, took place in Whippany, NJon May 19-21, 2003. This workshop, which was co-sponsored by the American Chemical Society-Medicinal Chemistry Division and the Society for Biomolecular Screening, was focused on prediction, measurement, and utilization of drug-like properties during lead selection. From this workshop arose the book entitled Pharmaceutical Profiling in Drug discovery for Lead Selection, which was edited by Ronald T. Borchardt, Edward H. Kerns, Christopher A. Lipinski, Dhiren R. Thakker and Binghe Wang and published by AAPS Press (Arlington, VA) in 2004. The second workshop entitled Optimizing the Drug-Like Properties of Leads in Drug Discovery took place in Parsippany, NJ on September 19-22, 2004. This workshop, which was co-sponsored by the American Chemical Society-Medicinal Chemistry Division, American Chemical Society-North Jersey Section, American Society for Clinical Pharmacology and Therapeutics, European Federation for Pharmaceutical Sciences, International Society for the study of Xenobiotics, and the Society of Toxicology, was focused on the optimization of the drug-like properties of leads in drug discovery. If the strategies and the methodologies presented at this workshop were to be adopted by pharmaceutical and biotechnology companies, it is the belief of the workshopbs organizers that more higher quality drug candidates would be advancing into preclinical and clinical development resulting in more efficacious and safer drugs.

Full Product Details

Author:   Ronald Borchardt ,  Edward Kerns ,  Michael Hageman
Publisher:   Springer
Imprint:   Springer
Volume:   40
Dimensions:   Width: 25.40cm , Height: 2.70cm , Length: 17.80cm
Weight:   0.907kg
ISBN:  

9780387513843


ISBN 10:   0387513841
Pages:   225
Publication Date:   01 January 1989
Audience:   General/trade ,  General
Format:   Undefined
Publisher's Status:   Unknown
Availability:   Out of stock   Availability explained

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