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. 2010 Jan 30;31(2):455-61.
doi: 10.1002/jcc.21334.

AutoDock Vina: improving the speed and accuracy of docking with a new scoring function, efficient optimization, and multithreading

Oleg Trott  1 Arthur J Olson
Affiliations

AutoDock Vina: improving the speed and accuracy of docking with a new scoring function, efficient optimization, and multithreading

"VSports最新版本" Oleg Trott et al. J Comput Chem. .

Abstract

AutoDock Vina, a new program for molecular docking and virtual screening, is presented. AutoDock Vina achieves an approximately two orders of magnitude speed-up compared with the molecular docking software previously developed in our lab (AutoDock 4), while also significantly improving the accuracy of the binding mode predictions, judging by our tests on the training set used in AutoDock 4 development. Further speed-up is achieved from parallelism, by using multithreading on multicore machines VSports手机版. AutoDock Vina automatically calculates the grid maps and clusters the results in a way transparent to the user. .

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"V体育官网入口" Figures

Figure 1
Figure 1
Weighted scoring function term combinations. Steric interactions; steric and hydrophobic interactions; and steric and hydrogen bonding interactions, using weights from table 1
Figure 2
Figure 2
RMSD of the predicted bound ligand conformation from the experimental one, showing the values for Vina and Autodock. The color encodes the number of active rotatable bonds
Figure 3
Figure 3
RMSD of the predicted bound ligand conformation from the experimental one. (Red +) Autodock; (Green ×) Vina. Abscissa shows the number of active rotatable bonds
Figure 4
Figure 4
Time, in minutes, taken by the multi-threaded Vina run, as a function of the number of heavy atoms in the ligand. The color encodes the number of active rotatable bonds
Figure 5
Figure 5
The fraction of the 190 test complexes for which RMSD < 2Å was achieved by AutoDock and Vina
Figure 6
Figure 6
Average time, in minutes per complex, taken by AutoDock, single-threaded Vina and Vina with 8-way multithreading. Machines with two quad-core 2.66GHz Xeon processors were used in the experiment. The time for AutoDock does not include the necessary initial AutoGrid run
Figure 7
Figure 7
Experimental and predicted free energies of binding (kcal/mol) for (a) AutoDock, (b) Vina. The color encodes the number of active rotatable bonds
See this image and copyright information in PMC

References

    1. Sousa SF, Fernandes PA, Ramos MJ. Protein-ligand docking: Current status and future challenges. Proteins-Structure Function and Bioinformatics. 2006 Oct 1;vol. 65:15–26. - PubMed
    1. Chang MW, Lindstrom W, Olson AJ, Belew RK. Analysis of HIV wild-type and mutant structures via in silico docking against diverse ligand libraries. Journal of Chemical Information and Modeling. 2007 May–Jun;vol. 47:1258–1262. - "VSports在线直播" PubMed
    1. Gilson MK, Zhou H-X. Calculation of protein-ligand binding affinities. Annual Review of Biophysics and Biomolecular Structure. 2007;vol. 36:21–42. - PubMed
    1. Gilson M, Given J, Bush B, McCammon J. The statistical-thermodynamic basis for computation of binding affinities: A critical review. Biophysical Journal. 1997 Mar;vol. 72:1047–1069. - PMC - PubMed
    1. Chang C-eA, Chen W, Gilson MK. Ligand configurational entropy and protein binding. Proceedings of the National Academy of Sciences of the United States of America. 2007 Jan 30;vol. 104:1534–1539. - PMC - PubMed

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