Optimization of biaryl piperidine and 4-amino-2-biarylurea MCH1 receptor antagonists using QSAR modeling, classification techniques and virtual screening

Journal of Computer-Aided Molecular Design - Tập 21 - Trang 251-267 - 2007
Georgia Melagraki1, Antreas Afantitis1,2, Haralambos Sarimveis1, Panayiotis A. Koutentis3, John Markopoulos4, Olga Igglessi-Markopoulou1
1School of Chemical Engineering, National Technical University of Athens, Athens, Greece
2Department of ChemoInformatics, NovaMechanics Ltd, Larnaca, Cyprus
3Department of Chemistry, University of Cyprus, Nicosia, Cyprus
4Department of Chemistry, University of Athens, Athens Greece

Tóm tắt

This paper presents the results of an optimization study on biaryl piperidine and 4-amino-2-biarylurea MCH1 receptor antagonists, which was accomplished by using quantitative-structure activity relationships (QSARs), classification and virtual screening techniques. First, a linear QSAR model was developed using Multiple Linear Regression (MLR) Analysis, while the Elimination Selection-Stepwise Regression (ES-SWR) method was adopted for selecting the most suitable input variables. The predictive activity of the model was evaluated using an external validation set and the Y-randomization technique. Based on the selected descriptors, the Support Vector Machines (SVM) classification technique was utilized to classify data into two categories: “actives” or “non-actives”. Several attempts were made to optimize the scaffold of most potent compounds by inducing various structural modifications. Potential derivatives with improved activities were identified, as they were classified “actives” by the SVM classifier. Their activities were estimated using the produced MLR model. A detailed analysis on the model applicability domain defined the compounds, whose estimations can be accepted with confidence.

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