Resum
A large virtual library of 125 396 HEPT analogues, built by combining all fragments present in the published 180-compound HEPT family, has been studied in terms of diversity criteria and the goodness of the 11 available standard diversity selection methods analyzed. All the algorithms under study, except Cell-based Density, have rank above a random selection of compounds, with Optimum and Standard Deviation based Binning and Cell-based Fraction algorithms being the best choices. Furthermore, analysis of the actually tested compounds has been performed to compare the traditional drug discovery methodology versus a rational selection of combinatorial libraries approach.
Idioma original | Anglès |
---|---|
Pàgines (de-a) | 199-207 |
Nombre de pàgines | 9 |
Revista | Journal of Chemical Information and Computer Sciences |
Volum | 43 |
Número | 1 |
DOIs | |
Estat de la publicació | Publicada - de gen. 2003 |