Journal ArticleDOI
Latest developments in molecular docking: 2010-2011 in review.
TLDR
The main developments in docking in this period, covered in this review, are receptor flexibility, solvation, fragment docking, postprocessing, docking into homology models, and docking comparisons.Abstract:
The aim of docking is to accurately predict the structure of a ligand within the constraints of a receptor binding site and to correctly estimate the strength of binding. We discuss, in detail, methodological developments that occurred in the docking field in 2010 and 2011, with a particular focus on the more difficult, and sometimes controversial, aspects of this promising computational discipline. The main developments in docking in this period, covered in this review, are receptor flexibility, solvation, fragment docking, postprocessing, docking into homology models, and docking comparisons. Several new, or at least newly invigorated, advances occurred in areas such as nonlinear scoring functions, using machine-learning approaches. This review is strongly focused on docking advances in the context of drug design, specifically in virtual screening and fragment-based drug design. Where appropriate, we refer readers to exemplar case studies.read more
Citations
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Journal ArticleDOI
PLIP: fully automated protein–ligand interaction profiler
TL;DR: The protein-ligand interaction profiler (PLIP) is presented, a novel web service for fully automated detection and visualization of relevant non-covalent protein–ligand contacts in 3D structures, freely available at projects.tu-dresden.de/plip-web.
Journal ArticleDOI
Comprehensive evaluation of ten docking programs on a diverse set of protein-ligand complexes: the prediction accuracy of sampling power and scoring power.
TL;DR: Overall, the ligand binding poses could be identified in most cases by the evaluated docking programs but the ranks of the binding affinities for the entire dataset could not be well predicted by most docking programs.
Journal ArticleDOI
DOCK 6: Impact of new features and current docking performance
William J. Allen,Trent E. Balius,Sudipto Mukherjee,Scott R. Brozell,Demetri T. Moustakas,P. Therese Lang,David A. Case,Irwin D. Kuntz,Robert C. Rizzo +8 more
TL;DR: This manuscript presents the latest algorithmic and methodological developments to the structure‐based design program DOCK 6.7 focused on an updated internal energy function, new anchor selection control, enhanced minimization options, a footprint similarity scoring function, a symmetry‐corrected root‐mean‐square deviation algorithm, a database filter, and docking forensic tools.
Journal ArticleDOI
Receptor–ligand molecular docking
TL;DR: The main topics and recent computational and methodological advances in protein–ligand docking are summarised, including protein flexibility, multiple ligand binding modes and the free-energy landscape profile for binding affinity prediction.
Journal ArticleDOI
Oncogenic protein interfaces: small molecules, big challenges
TL;DR: Some of the latest techniques to discover modulators of protein–protein interactions are described and how current drug discovery approaches have been adapted to successfully target these interfaces are described.
References
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Journal ArticleDOI
A python-based docking program utilizing a receptor bound ligand shape: PythDock.
TL;DR: PythDock is a heuristic docking program that uses Python programming language with a simple scoring function and a population based search engine that could be a useful tool to study ligand-receptor interactions and could also be beneficial in structure based drug design.
Journal ArticleDOI
Assessment of a novel scoring method based on solvent accessible surface area descriptors.
TL;DR: A novel scoring algorithm based on unique solvent accessible surface area (SASA) descriptors was comparatively evaluated for its database enrichment potential against the virtual screening methods GOLD and Glide and found an outstanding robustness to produce satisfactory early enrichments for a large variety of target classes.
Journal ArticleDOI
VSDK: Virtual screening of small molecules using AutoDock Vina on Windows platform.
Natsumi Baba,Eiichi Akaho +1 more
TL;DR: A virtual screening application system, named VSDK Virtual Screening by Docking, which can function under the Windows platform, which is a user-friendly, flexible, and versatile tool which can be used by users who are familiar with Windows OS.
Journal ArticleDOI
PLS-DA - Docking Optimized Combined Energetic Terms (PLSDA-DOCET) protocol: a brief evaluation.
TL;DR: The target oriented consensus technique using the energetic terms of several scoring functions, denoted PLSDA-DOCET, outperformed the other docking approaches regarding simple retrieval and scaffold-hopping and was validated on an external test set.
Journal ArticleDOI
Prediction of protein-ligand binding affinities using multiple instance learning.
Reiji Teramoto,Hisashi Kashima +1 more
TL;DR: A new method called multiple instance regression based scoring (MIRS) that incorporates unbound ligand conformations using multiple scoring functions to predict protein-ligand binding affinity directly and will accelerate efficient lead optimization on structure-based drug design and provide a new direction to designing of new scoring score functions.
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