Goetz | Cyclic Peptide Design | Buch | 978-1-4939-9506-6 | www.sack.de

Buch, Englisch, 332 Seiten, Format (B × H): 178 mm x 254 mm, Gewicht: 648 g

Reihe: Methods in Molecular Biology

Goetz

Cyclic Peptide Design


1. Auflage 2019
ISBN: 978-1-4939-9506-6
Verlag: Springer

Buch, Englisch, 332 Seiten, Format (B × H): 178 mm x 254 mm, Gewicht: 648 g

Reihe: Methods in Molecular Biology

ISBN: 978-1-4939-9506-6
Verlag: Springer

This book covers strategies to improve cell permeability, intestinal permeability, and metabolic stability, which are the typical liabilities associated with cyclic peptides, to enhance protein-protein recognition, and to build upon nature’s cyclic peptides and macrocycles. Chapters also cover key peptide screening and display strategies, as well as important synthetic approaches towards cyclic and helical peptides. Cyclic peptides have become of significant importance as chemical tools in biology and drug discovery, since this class of chemicals has become a credible alternative source of new drug leads on par with traditional small molecules. As a part of the Methods in Molecular Biology series, this collection includes the kind of detail and implementation advice to aid researchers in the field. 
Authoritative and cutting-edge, Cyclic Peptide Design serves as a critical resource and go-to reference for researchers within the pharmaceutical industry, as well as scientists and students in the bioorganic, medicinal, and natural product chemistry fields.
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Zielgruppe

Professional/practitioner

Autoren/Hrsg.

Goetz, Gilles

Fachgebiete

Weitere Infos & Material

Design Principles for Intestinal Permeability of Cyclic Peptides.- Strategies to Enhance Metabolic Stabilities.- Designing Cell-Permeable Macrocyclic Peptides.- Computational Methods for Studying Conformational Behaviors of Cyclic Peptides.- Computational Opportunities and Challenges in Finding Cyclic Peptide Modulators of Protein-Protein Interactions.- Design of Cyclic Peptides as Protein Recognition Motifs.- Design and Synthetic Strategies for Helical Peptides.- Click Chemistry for Cyclic Peptides Drug Design.- Frontier between Cyclic Peptides and Macrocycles.- Building upon Nature’s Framework: Overview of Key Strategies towards Increasing Drug-Like Properties of Natural Product Cyclopeptides and Macrocycles.- Design of Oxytocin Analogs.- DNA-Encoded Macrocyclic Peptide Library.- Peptide Display Technologies.- Discovery of Functional Macrocyclic Peptides by Means of the RaPID System.- Genetic Selections with SICLOPPS Libraries: Towards the Identification of Novel Protein-Protein Interaction Inhibitors and Chemical Tools.

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