ABSTRACT: Virtual ligand screening is an integral part of the modern drug discovery process. Traditional ligand-based, virtual screening approaches are fast but require a set of structurally diverse ligands known to bind to the target. Traditional structure-based approaches require high-resolution target protein structures and are computationally demanding. In contrast, the recently developed threading/structure-based FINDSITE-based approaches have the advantage that they are as fast as traditional ligand-based approaches and yet overcome the limitations of traditional ligand- or structure-based approaches. These new methods can use predicted low-resolution structures and infer the likelihood of a ligand binding to a target by utilizing lig...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
Background: Many of solved tertiary structures of unknown functions do not have global sequence and ...
Computational approaches for predicting protein–ligand interactions can facilitate drug lead discove...
The detection of ligand-binding sites is often the starting point for protein function identificatio...
Ligand virtual screening is a widely used tool to assist in new pharmaceutical discovery. In practic...
Ligand virtual screening is a widely used tool to assist in new pharmaceutical discovery. In practic...
We have developed FINDSITE<sup>X</sup>, an extension of FINDSITE, a protein threading based algorith...
©2009 Brylinski, Skolnick. This is an open-access article distributed under the terms of the Creativ...
We have developed a new computational algorithm for de novo identification of protein-ligand bindin...
After the onset of the genomic era, the detection of ligand binding sites in proteins has emerged ov...
After the onset of the genomic era, the detection of ligand binding sites in proteins has emerged ov...
There are several methods for virtual screening of databases of small organic compounds to find tigh...
Modern drug discovery has evolved into a rational design paradigm, where the vast chemical space is ...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
Background: Many of solved tertiary structures of unknown functions do not have global sequence and ...
Computational approaches for predicting protein–ligand interactions can facilitate drug lead discove...
The detection of ligand-binding sites is often the starting point for protein function identificatio...
Ligand virtual screening is a widely used tool to assist in new pharmaceutical discovery. In practic...
Ligand virtual screening is a widely used tool to assist in new pharmaceutical discovery. In practic...
We have developed FINDSITE<sup>X</sup>, an extension of FINDSITE, a protein threading based algorith...
©2009 Brylinski, Skolnick. This is an open-access article distributed under the terms of the Creativ...
We have developed a new computational algorithm for de novo identification of protein-ligand bindin...
After the onset of the genomic era, the detection of ligand binding sites in proteins has emerged ov...
After the onset of the genomic era, the detection of ligand binding sites in proteins has emerged ov...
There are several methods for virtual screening of databases of small organic compounds to find tigh...
Modern drug discovery has evolved into a rational design paradigm, where the vast chemical space is ...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
International audienceBACKGROUND: Virtual screening methods are now well established as effective to...
Background: Many of solved tertiary structures of unknown functions do not have global sequence and ...
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