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The scoring bias in reverse docking and the score normalization strategy to improve success rate of target fishing. | LitMetric

The scoring bias in reverse docking and the score normalization strategy to improve success rate of target fishing.

PLoS One

State Key Laboratory of Natural and Biomimetic Drugs, School of Pharmaceutical Sciences, Peking University, Beijing, P. R. China.

Published: August 2017

AI Article Synopsis

  • Target fishing uses reverse docking to find potential proteins that bind to specific ligands, but current scoring methods often misidentify true targets due to bias based on protein pocket properties.
  • A large-scale study involving 5,000 molecules and 100 proteins revealed that interference proteins consistently caused false positives across three docking programs (DOCK, Glide, AutoDock Vina) due to their larger contact areas and higher hydrophobicity.
  • Implementing a score normalization method effectively reduced scoring bias, leading to a 21.5% improvement in target prediction accuracy for Glide, while showing inconsistent results for DOCK and AutoDock Vina.

Article Abstract

Target fishing often relies on the use of reverse docking to identify potential target proteins of ligands from protein database. The limitation of reverse docking is the accuracy of current scoring funtions used to distinguish true target from non-target proteins. Many contemporary scoring functions are designed for the virtual screening of small molecules without special optimization for reverse docking, which would be easily influenced by the properties of protein pockets, resulting in scoring bias to the proteins with certain properties. This bias would cause lots of false positives in reverse docking, interferring the identification of true targets. In this paper, we have conducted a large-scale reverse docking (5000 molecules to 100 proteins) to study the scoring bias in reverse docking by DOCK, Glide, and AutoDock Vina. And we found that there were actually some frequency hits, namely interference proteins in all three docking procedures. After analyzing the differences of pocket properties between these interference proteins and the others, we speculated that the interference proteins have larger contact area (related to the size and shape of protein pockets) with ligands (for all three docking programs) or higher hydrophobicity (for Glide), which could be the causes of scoring bias. Then we applied the score normalization method to eliminate this scoring bias, which was effective to make docking score more balanced between different proteins in the reverse docking of benchmark dataset. Later, the Astex Diver Set was utilized to validate the effect of score normalization on actual cases of reverse docking, showing that the accuracy of target prediction significantly increased by 21.5% in the reverse docking by Glide after score normalization, though there was no obvious change in the reverse docking by DOCK and AutoDock Vina. Our results demonstrate the effectiveness of score normalization to eliminate the scoring bias and improve the accuracy of target prediction in reverse docking. Moreover, the properties of protein pockets causing scoring bias to certain proteins we found here can provide the theory basis to further optimize the scoring functions of docking programs for future research.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5308821PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0171433PLOS

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