posted on 2013-12-23, 00:00authored byYanmin Zhang, Shangyan Yang, Yu Jiao, Haichun Liu, Haoliang Yuan, Shuai Lu, Ting Ran, Sihui Yao, Zhipeng Ke, Jinxing Xu, Xiao Xiong, Yadong Chen, Tao Lu
In recent years, various virtual
screening (VS) tools have been
developed, and many successful screening campaigns have been showcased.
However, whether by conventional molecular docking or pharmacophore
screening, the selection of virtual hits is based on the ranking of
compounds by scoring functions or fit values, which remains the bottleneck
of VS due to insufficient accuracy. As the limitations of individual
methods persist, a comprehensive comparison and integration of different
methods may provide insights into selecting suitable methods for VS.
Here, we evaluated the performance of molecular docking, fingerprint-based
2D similarity and multicomplex pharmacophore in an individual and
a combined manner, through a retrospective VS study on VEGFR-2 inhibitors.
An integrated two-layer workflow was developed and validated through
VS of VEGFR-2 inhibitors against the DUD-E database, which demonstrated
improved VS performance through a ligand-based method ECFP_4, followed
by molecular docking, and then a strict multicomplex pharmacophore.
Through a retrospective comparison with six published papers, this
integrated approach outperformed 43 out of 45 methods, indicating
a great effectiveness. This kind of integrated VS approach can be
extended to other targets for the screening and discovery of inhibitors.