Abstract

Ligand-based Virtual Screening (VS) methods aim at identifying molecules with a similar activity profile across phenotypic and macromolecular targets to that of a query molecule used as search template. VS using 3D similarity methods have the advantage of biasing this search toward active molecules with innovative chemical scaffolds, which are highly sought after in drug design to provide novel leads with improved properties over the query molecule (e.g. patentable, of lower toxicity or increased potency). Ultrafast Shape Recognition (USR) has demonstrated excellent performance in the discovery of molecules with previously-unknown phenotypic or target activity, with retrospective studies suggesting that its pharmacophoric extension (USRCAT) should obtain even better hit rates once it is used prospectively. Here we present USR-VS (http://usr.marseille.inserm.fr/), the first web server using these two validated ligand-based 3D methods for large-scale prospective VS. In about 2 s, 93.9 million 3D conformers, expanded from 23.1 million purchasable molecules, are screened and the 100 most similar molecules among them in terms of 3D shape and pharmacophoric properties are shown. USR-VS functionality also provides interactive visualization of the similarity of the query molecule against the hit molecules as well as vendor information to purchase selected hits in order to be experimentally tested.

Highlights

  • Ultrafast Shape Recognition [1] (USR) is a molecular shape similarity technique enabling extremely rapid search for molecules with similar 3D shapes

  • In USR, each shape is encoded by a vector of 12 geometrical features derived from four strategically-located reference points with similar locations in similar molecules, providing a common framework for the comparison [2]

  • This paper describes USR-VS, a user-friendly USRbased web server to perform large-scale ligand-based Virtual Screening (VS), which is oriented to the prospective validation of the obtained results

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Summary

Introduction

Ultrafast Shape Recognition [1] (USR) is a molecular shape similarity technique enabling extremely rapid search for molecules with similar 3D shapes. This paper describes USR-VS, a user-friendly USRbased web server to perform large-scale ligand-based Virtual Screening (VS), which is oriented to the prospective validation of the obtained results.

Results
Conclusion

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