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| Author | : Kira A. Armacost |
| Publisher | : |
| Total Pages | : |
| Release | : 2021 |
| Genre | : Drug development |
| ISBN | : 9780841298057 |
"This book is about Free Energy Methods in Drug Discovery: Current State and Future Directions"--
| Author | : Kira A. Armacost |
| Publisher | : |
| Total Pages | : |
| Release | : 2021 |
| Genre | : Drug development |
| ISBN | : 9780841298064 |
"This book is about Free Energy Methods in Drug Discovery: Current State and Future Directions"--
| Author | : Christophe Chipot |
| Publisher | : Springer Science & Business Media |
| Total Pages | : 528 |
| Release | : 2007-01-08 |
| Genre | : Language Arts & Disciplines |
| ISBN | : 3540384472 |
Free energy constitutes the most important thermodynamic quantity to understand how chemical species recognize each other, associate or react. Examples of problems in which knowledge of the underlying free energy behaviour is required, include conformational equilibria and molecular association, partitioning between immiscible liquids, receptor-drug interaction, protein-protein and protein-DNA association, and protein stability. This volume sets out to present a coherent and comprehensive account of the concepts that underlie different approaches devised for the determination of free energies. The reader will gain the necessary insight into the theoretical and computational foundations of the subject and will be presented with relevant applications from molecular-level modelling and simulations of chemical and biological systems. Both formally accurate and approximate methods are covered using both classical and quantum mechanical descriptions. A central theme of the book is that the wide variety of free energy calculation techniques available today can be understood as different implementations of a few basic principles. The book is aimed at a broad readership of graduate students and researchers having a background in chemistry, physics, engineering and physical biology.
| Author | : M. Rami Reddy |
| Publisher | : Springer Science & Business Media |
| Total Pages | : 420 |
| Release | : 2001-12-31 |
| Genre | : Medical |
| ISBN | : 9780306466762 |
Free energy calculations represent the most accurate computational method available for predicting enzyme inhibitor binding affinities. Advances in computer power in the 1990s enabled the practical application of these calculations in rationale drug design. This book represents the first comprehensive review of this growing area of research and covers the basic theory underlying the method, numerous state of the art strategies designed to improve throughput and dozen examples wherein free energy calculations were used to design and evaluate potential drug candidates.
| Author | : Lin Song |
| Publisher | : |
| Total Pages | : 169 |
| Release | : 2020 |
| Genre | : Electronic dissertations |
| ISBN | : 9781083282941 |
With the increasing power of computers, computational studies have become more and more significant in drug discovery. High binding free energy is one of the major requirements for an effective drug molecule, hence much effort has been spent to develop fast and accurate computational free energy methods. In this thesis, different free energy methods, i.e. umbrella sampling, thermodynamic integration, and double decoupling method, are applied to different systems related to drug discovery. For the first study, umbrella sampling studies are performed to calculate the absolute binding free energies of host-guest systems which serve as great model systems to assess free energy methods due to the small size of the systems, etc. We find that benchmarking our method with known systems can significantly improve the results for the unknown systems: the overall RMSE of the binding free energy versus experiment is reduced from 5.59 kcal/mol to 2.36 kcal/mol. The source of error could be from the un-optimized force constants used in umbrella sampling (hence possibly poor window overlaps), as well as force field, sampling issues, etc. Our results ranked 4th best in the Statistical Assessment of the Modeling of Proteins and Ligands (SAMPL6) blind challenge. For the second study, GPU accelerated thermodynamic integration (GPU-TI) is used to compute the relative binding free energies of a protein-ligand dataset originally assembled by Schrodinger, Inc. The calculations of relative binding free energies between different ligands are the typical process in the lead optimization of computer-aided drug discovery. In our study using GPU-TI from AMBER 18 with the AMBER14SB/GAFF1.8 force field, we obtained an overall MUE of 1.17 kcal/mol and an overall RMSE of 1.50 kcal/mol for the 330 perturbations contained in this data set. They are comparable to the overall MUE of 0.9 kcal/mol and RMSE of 1.14 kcal/mol using their GPU free energy code (FEP+) and the OPLS2.1 force field combined with the REST2 enhanced sampling by Schrodinger, Inc. Notably, after we published our work, several other research groups reported their benchmarking results on the other free energy software using the same dataset.The third study of this thesis focuses on modeling the thermodynamics of transition metal (TM) ions binding to a protein. TM ions are very common in biology and are important in drug discovery as well, because many TM ions are in the active site of the protein where the inhibitors bind, for example, the histone deacetylase. While the structural details of TMs bound to metalloproteins are generally well understood via experimental and computational means; studies accurately describing the thermodynamics of TM ion binding are less common. Herein, we demonstrate that we can obtain accurate structural and absolute binding free energies of Co2+ and Ni2+ to the enzyme glyoxalase I (GlxI) using an optimized 12-6-4 (m12-6-4) potential. Optimizing the 12-6-4 potential to accurately model the interactions between the TMs and the binding site residues, as well as protonation state changes associated with TMs (un)binding, are found to be crucial. Given the success of this study, we are now in a position to explore more complicated processes associated with TM-based drug discovery.
| Author | : Kenneth M. Merz |
| Publisher | : Cambridge University Press |
| Total Pages | : 289 |
| Release | : 2010-05-31 |
| Genre | : Medical |
| ISBN | : 0521887232 |
This book provides a complete snapshot of various experimental approaches to structure-based and ligand-based drug design and is illustrated with more than 200 images.
| Author | : Javier Luque |
| Publisher | : Royal Society of Chemistry |
| Total Pages | : 443 |
| Release | : 2012 |
| Genre | : Medical |
| ISBN | : 1849733538 |
This title covers a wide range of topics relevant to the development of drugs. It provides a comprehensive description of the major methodological strategies available for rational drug discovery.
| Author | : Francesco L. Gervasio |
| Publisher | : John Wiley & Sons |
| Total Pages | : 368 |
| Release | : 2019-04-29 |
| Genre | : Medical |
| ISBN | : 3527342656 |
A guide to applying the power of modern simulation tools to better drug design Biomolecular Simulations in Structure-based Drug Discovery offers an up-to-date and comprehensive review of modern simulation tools and their applications in real-life drug discovery, for better and quicker results in structure-based drug design. The authors describe common tools used in the biomolecular simulation of drugs and their targets and offer an analysis of the accuracy of the predictions. They also show how to integrate modeling with other experimental data. Filled with numerous case studies from different therapeutic fields, the book helps professionals to quickly adopt these new methods for their current projects. Experts from the pharmaceutical industry and academic institutions present real-life examples for important target classes such as GPCRs, ion channels and amyloids as well as for common challenges in structure-based drug discovery. Biomolecular Simulations in Structure-based Drug Discovery is an important resource that: -Contains a review of the current generation of biomolecular simulation tools that have the robustness and speed that allows them to be used as routine tools by non-specialists -Includes information on the novel methods and strategies for the modeling of drug-target interactions within the framework of real-life drug discovery and development -Offers numerous illustrative case studies from a wide-range of therapeutic fields -Presents an application-oriented reference that is ideal for those working in the various fields Written for medicinal chemists, professionals in the pharmaceutical industry, and pharmaceutical chemists, Biomolecular Simulations in Structure-based Drug Discovery is a comprehensive resource to modern simulation tools that complement and have the potential to complement or replace laboratory assays for better results in drug design.
| Author | : Jean-Paul Renaud |
| Publisher | : John Wiley & Sons |
| Total Pages | : 1367 |
| Release | : 2020-01-09 |
| Genre | : Medical |
| ISBN | : 1118900502 |
With the most comprehensive and up-to-date overview of structure-based drug discovery covering both experimental and computational approaches, Structural Biology in Drug Discovery: Methods, Techniques, and Practices describes principles, methods, applications, and emerging paradigms of structural biology as a tool for more efficient drug development. Coverage includes successful examples, academic and industry insights, novel concepts, and advances in a rapidly evolving field. The combined chapters, by authors writing from the frontlines of structural biology and drug discovery, give readers a valuable reference and resource that: Presents the benefits, limitations, and potentiality of major techniques in the field such as X-ray crystallography, NMR, neutron crystallography, cryo-EM, mass spectrometry and other biophysical techniques, and computational structural biology Includes detailed chapters on druggability, allostery, complementary use of thermodynamic and kinetic information, and powerful approaches such as structural chemogenomics and fragment-based drug design Emphasizes the need for the in-depth biophysical characterization of protein targets as well as of therapeutic proteins, and for a thorough quality assessment of experimental structures Illustrates advances in the field of established therapeutic targets like kinases, serine proteinases, GPCRs, and epigenetic proteins, and of more challenging ones like protein-protein interactions and intrinsically disordered proteins
| Author | : Sergio Decherchi |
| Publisher | : Frontiers Media SA |
| Total Pages | : 119 |
| Release | : 2021-06-08 |
| Genre | : Science |
| ISBN | : 2889668630 |
Dr. Sergio Decherchi and Dr. Andrea Cavalli are co-founders of BiKi Technologies s.r.l. - a company that commercializes a Molecular Dynamics-based software suite for drug discovery. All other Topic Editors declare no competing interests with regards to the Research Topic subject.
