The Design of Covalent-Based Inhibitors

The Design of Covalent-Based Inhibitors
Author :
Publisher : Elsevier
Total Pages : 298
Release :
ISBN-10 : 9780128216897
ISBN-13 : 0128216891
Rating : 4/5 (97 Downloads)

Synopsis The Design of Covalent-Based Inhibitors by : Richard A Ward

Annual Report on Medicinal Chemistry series, highlights new advances in the field with this new volume presenting interesting chapters. Each chapter is written by an international board of authors. Provides the authority and expertise of leading contributors from an international board of authors Presents the latest release in the Annual Report on Medicinal Chemistry series Updated release includes the latest information on The Design of Covalent-Based Inhibitors

Biomedical Chemistry

Biomedical Chemistry
Author :
Publisher : Walter de Gruyter GmbH & Co KG
Total Pages : 361
Release :
ISBN-10 : 9783110468755
ISBN-13 : 3110468751
Rating : 4/5 (55 Downloads)

Synopsis Biomedical Chemistry by : Nuno Vale

Biomedical Chemistry provides readers with an understanding of how fundamental chemical concepts are used to combat some diseases. The authors explain the interdisciplinary relationship of chemistry with biology, physics, pharmacy and medicine. The results of chemical research can be applied to understand chemical processes in cells and in the body, and new methods for drug transportation. Also, basic chemical ideas and determination of disease etiology are approached by developing techniques to ensure optimum interaction between drugs and human cells. This Book is an excellent resource for students and researchers in health-related fields with frontier topics in medicinal and pharmaceutical chemistry, organic chemistry and biochemistry.

The Design of Covalent-Based Inhibitors

The Design of Covalent-Based Inhibitors
Author :
Publisher : Academic Press
Total Pages : 300
Release :
ISBN-10 : 9780128232460
ISBN-13 : 0128232463
Rating : 4/5 (60 Downloads)

Synopsis The Design of Covalent-Based Inhibitors by :

Annual Report on Medicinal Chemistry series, highlights new advances in the field with this new volume presenting interesting chapters. Each chapter is written by an international board of authors. - Provides the authority and expertise of leading contributors from an international board of authors - Presents the latest release in the Annual Report on Medicinal Chemistry series - Updated release includes the latest information on The Design of Covalent-Based Inhibitors

Activity-Based Protein Profiling

Activity-Based Protein Profiling
Author :
Publisher : Springer
Total Pages : 420
Release :
ISBN-10 : 9783030111434
ISBN-13 : 3030111431
Rating : 4/5 (34 Downloads)

Synopsis Activity-Based Protein Profiling by : Benjamin F. Cravatt

This volume provides a collection of contemporary perspectives on using activity-based protein profiling (ABPP) for biological discoveries in protein science, microbiology, and immunology. A common theme throughout is the special utility of ABPP to interrogate protein function and small-molecule interactions on a global scale in native biological systems. Each chapter showcases distinct advantages of ABPP applied to diverse protein classes and biological systems. As such, the book offers readers valuable insights into the basic principles of ABPP technology and how to apply this approach to biological questions ranging from the study of post-translational modifications to targeting bacterial effectors in host-pathogen interactions.

Fragment-Based Drug Discovery

Fragment-Based Drug Discovery
Author :
Publisher : Royal Society of Chemistry
Total Pages : 314
Release :
ISBN-10 : 9781782625650
ISBN-13 : 1782625658
Rating : 4/5 (50 Downloads)

Synopsis Fragment-Based Drug Discovery by : Steven Howard

Fragment-based drug discovery is a rapidly evolving area of research, which has recently seen new applications in areas such as epigenetics, GPCRs and the identification of novel allosteric binding pockets. The first fragment-derived drug was recently approved for the treatment of melanoma. It is hoped that this approval is just the beginning of the many drugs yet to be discovered using this fascinating technique. This book is written from a Chemist's perspective and comprehensively assesses the impact of fragment-based drug discovery on a wide variety of areas of medicinal chemistry. It will prove to be an invaluable resource for medicinal chemists working in academia and industry, as well as anyone interested in novel drug discovery techniques.

Structure-based Design of Drugs and Other Bioactive Molecules

Structure-based Design of Drugs and Other Bioactive Molecules
Author :
Publisher : John Wiley & Sons
Total Pages : 474
Release :
ISBN-10 : 9783527333653
ISBN-13 : 3527333657
Rating : 4/5 (53 Downloads)

Synopsis Structure-based Design of Drugs and Other Bioactive Molecules by : Arun K. Ghosh

Drug design is a complex, challenging and innovative research area. Structure-based molecular design has transformed the drug discovery approach in modern medicine. Traditionally, focus has been placed on computational, structural or synthetic methods only in isolation. This one-of-akind guide integrates all three skill sets for a complete picture of contemporary structure-based design. This practical approach provides the tools to develop a high-affinity ligand with drug-like properties for a given drug target for which a high-resolution structure exists. The authors use numerous examples of recently developed drugs to present "best practice" methods in structurebased drug design with both newcomers and practicing researchers in mind. By way of a carefully balanced mix of theoretical background and case studies from medicinal chemistry applications, readers will quickly and efficiently master the basic skills of successful drug design. This book is aimed at new and active medicinal chemists, biochemists, pharmacologists, natural product chemists and those working in drug discovery in the pharmaceutical industry. It is highly recommended as a desk reference to guide students in medicinal and chemical sciences as well as to aid researchers engaged in drug design today.

The Organic Chemistry of Drug Design and Drug Action

The Organic Chemistry of Drug Design and Drug Action
Author :
Publisher : Elsevier
Total Pages : 650
Release :
ISBN-10 : 9780080513379
ISBN-13 : 0080513379
Rating : 4/5 (79 Downloads)

Synopsis The Organic Chemistry of Drug Design and Drug Action by : Richard B. Silverman

Standard medicinal chemistry courses and texts are organized by classes of drugs with an emphasis on descriptions of their biological and pharmacological effects. This book represents a new approach based on physical organic chemical principles and reaction mechanisms that allow the reader to extrapolate to many related classes of drug molecules. The Second Edition reflects the significant changes in the drug industry over the past decade, and includes chapter problems and other elements that make the book more useful for course instruction. - New edition includes new chapter problems and exercises to help students learn, plus extensive references and illustrations - Clearly presents an organic chemist's perspective of how drugs are designed and function, incorporating the extensive changes in the drug industry over the past ten years - Well-respected author has published over 200 articles, earned 21 patents, and invented a drug that is under consideration for commercialization

Handbook of In Vivo Chemistry in Mice

Handbook of In Vivo Chemistry in Mice
Author :
Publisher : John Wiley & Sons
Total Pages : 560
Release :
ISBN-10 : 9783527344321
ISBN-13 : 3527344322
Rating : 4/5 (21 Downloads)

Synopsis Handbook of In Vivo Chemistry in Mice by : Katsunori Tanaka

Provides timely, comprehensive coverage of in vivo chemical reactions within live animals This handbook summarizes the interdisciplinary expertise of both chemists and biologists performing in vivo chemical reactions within live animals. By comparing and contrasting currently available chemical and biological techniques, it serves not just as a collection of the pioneering work done in animal-based studies, but also as a technical guide to help readers decide which tools are suitable and best for their experimental needs. The Handbook of In Vivo Chemistry in Mice: From Lab to Living System introduces readers to general information about live animal experiments and detection methods commonly used for these animal models. It focuses on chemistry-based techniques to develop selective in vivo targeting methodologies, as well as strategies for in vivo chemistry and drug release. Topics include: currently available mouse models; biocompatible fluorophores; radionuclides for radiodiagnosis/radiotherapy; live animal imaging techniques such as positron emission tomography (PET) imaging; magnetic resonance imaging (MRI); ultrasound imaging; hybrid imaging; biocompatible chemical reactions; ligand-directed nucleophilic substitution chemistry; biorthogonal prodrug release strategies; and various selective targeting strategies for live animals. -Completely covers current techniques of in vivo chemistry performed in live animals -Describes general information about commonly used live animal experiments and detection methods -Focuses on chemistry-based techniques to develop selective in vivo targeting methodologies, as well as strategies for in vivo chemistry and drug release -Places emphasis on material properties required for the development of appropriate compounds to be used for imaging and therapeutic purposes in preclinical applications Handbook of In Vivo Chemistry in Mice: From Lab to Living System will be of great interest to pharmaceutical chemists, life scientists, and organic chemists. It will also appeal to those working in the pharmaceutical and biotechnology industries.

Inhibitors of Protein–Protein Interactions

Inhibitors of Protein–Protein Interactions
Author :
Publisher : Royal Society of Chemistry
Total Pages : 357
Release :
ISBN-10 : 9781788015691
ISBN-13 : 178801569X
Rating : 4/5 (91 Downloads)

Synopsis Inhibitors of Protein–Protein Interactions by : Ali Tavassoli

Protein-protein interactions (PPI) are at the heart of the majority of cellular processes, and are frequently dysregulated or usurped in disease. Given this central role, the inhibition of PPIs has been of significant interest as a means of treating a wide variety of diseases. However, there are inherent challenges in developing molecules capable of disrupting the relatively featureless and large interfacial areas involved. Despite this, there have been a number of successes in this field in recent years using both traditional drug discovery approaches and innovative, interdisciplinary strategies using novel chemical scaffolds. This book comprehensively covers the various aspects of PPI inhibition, encompassing small molecules, peptidomimetics, cyclic peptides, stapled peptides and macrocycles. Illustrated throughout with successful case studies, this book provides a holistic, cutting-edge view of the subject area and is ideal for chemical biologists and medicinal chemists interested in developing PPI inhibitors.

Endocrine FGFs and Klothos

Endocrine FGFs and Klothos
Author :
Publisher : Springer Science & Business Media
Total Pages : 250
Release :
ISBN-10 : 9781461408871
ISBN-13 : 1461408873
Rating : 4/5 (71 Downloads)

Synopsis Endocrine FGFs and Klothos by : Makoto Kuro-o

Fibroblast growth factors (FGFs) have been recognized primarily as autocrine/paracrine factors that regulate embryonic development and organogenesis. However, recent studies have revealed that some FGFs function as endocrine factors and regulate various metabolic processes in adulthood. Such FGFs, collectively called endocrine FGFs, are comprised of three members (FGF15/19, FGF21, and FGF23: FGF15 is the mouse ortholog of human FGF19). These endocrine FGFs share a common structural feature that enables the endocrine mode of action at the expense of the affinity to FGF receptors. To restore the affinity to FGF receptors in their target organs, the endocrine FGFs have designated the Klotho family of transmembrane proteins as obligate co-receptors. By expressing Klothos in a tissue-specific manner, this unique co-receptor system also enables the endocrine FGFs to specify their target organs among many tissues that express FGF receptors.