Predicting opioid receptor binding affinity of pharmacologically unclassified designer substances using molecular docking
Fig 4
Fentanyl analog binding prediction and classification.
Scatterplot of the experimentally determined binding affinity, Ki, with the ADS from the molecular docking procedure of the 8 fentanyl analogs (shown as diamonds). The grey, shaded regions display the sub-nM, 1–100 nM, and greater than 100 nM binding concentration regimes used to classify the predicted binding strength of new drugs. N-methyl fentanyl (blue), fentanyl (purple), carfentanil (green) and lofentanil (red) are presented with colored diamonds to demonstrate the method’s ability to separate fentanyl analogs into the proper binding concentration regimes. The remaining black diamonds represent the 4 other fentanyl analogs that were docked and scored.