P-gp Substrates: Difference between revisions

Experimental data

There are many in vitro and in vivo tests used in P-gp specificity studies that often produce contradictive results. P-gp specificity model is based on the data collected from scientific literature. The following assays for substrates were considered:

• In vitro polarized transport across P-gp expressing cell monolayers
• In vivo BBB models with P-gp knock-out animals, P-gp mediated drug resistance.

The respective assays for inhibitors were as follows:

• Drug efflux inhibition across/out of P-gp expressing cells
• MDR reversion.

The original data set for P-gp substrates contained >1,000 compounds, for inhibitors >1,500 compounds. In v. 2024, the P-gp substrate specificity training set has been expanded to almost 3,500 compounds with exact or censored ER data. About 2,900 of these can be unequivocally classified as P-gp substrates or non-substrates at a threshold of ER = 2, and the respective compounds were used to construct the updated Self-training library of the 'general substrate specificity' GALAS model.

Reference database

Percepta includes a browsable P-gp DB comprised of 2,290 compounds with experimental data related to their interactions with P-gp. Each compound in the DB is classified as a P-gp substrate or non-substrate (inconclusive or contradictive data are marked as Yes/No or No/Yes in the 'Substrate field) and efficiency of P-gp mediated transport is provided for substrates. High efficiency describes compounds that are transported with the rate similar to the best substrates (vinblastine, daunorubicin, paclitaxel). Similarly, drugs comprising the database are classified according to their Inhibitor liability. Potency field denotes effectivity of P-gp inhibition, High potency representing compounds that inhibit P-gp as good as standard inhibitor verapamil or even better.

In the Assays section, the methods that were used in the analysis of P-gp substrate/inhibitor specificity are listed:

• Substrate (in vitro transport assay) – polarized transport of drugs across P-gp expressing cell monolayers or decreased drug accumulation in MDR cells
• Substrate (in vivo BBB models) – increased distribution of drugs to the brain in P-gp deficient (mdr1a/b(-/-)) mice
• P-gp mediated resistance – P-gp overexpressing (MDR) cells demonstrate resistance to the drug
• Drug efflux inhibition – inhibition of drug efflux in P-gp expressing cells.
• MDR reversion – sensitization of P-gp expressing cells to “MDR profile” drugs (taxanes, anthracyclines, vinca alkaloids)
• P-gp ATPase modulation – activation or inhibition of P-gp ATPase. This assay does not differentiate P-gp substrates and inhibitors.

Model features & prediction accuracy

The predictive models of P-gp substrate specificity were derived using GALAS (Global, Adjusted Locally According to Similarity) modeling methodology (please refer to [1] for more details).

Each GALAS model consists of two parts:

• Global baseline statistical model employing binomial PLS with multiple bootstrapping using a predefined set of fragmental descriptors, that reflects general trends in P-gp substrate specificity.
• Similarity-based routine that performs local correction of baseline predictions taking into account the differences between baseline and experimental values for the most similar training set compounds.

GALAS methodology also provides the basis for estimating reliability of predictions by the means of calculated Reliability Index (RI) value that takes into account:

• Similarity of tested compound to the training set molecules (prediction is unreliable if no similar compounds have been found).
• Consistence of experimental values and baseline model prediction for the most similar compounds from the training set (discrepant data for similar molecules, i.e. alternating P-gp substrates and non-substrates lead to lower RI values).

Reliability Index ranges from 0 to 1 (0 corresponds to a completely unreliable, and 1 - a highly reliable prediction) and serves as an indication whether a submitted compound falls within the Model Applicability Domain. Compounds obtaining predictions RI < 0.3 are considered outside of the Applicability Domain of the model.

The presented method also forms the basis of model Trainability. 'Trainable model' methodology addresses the issue of the chemical space of ‘in-house’ libraries being considerably wider than that of publicly available data which results in limited applicability of most third-party QSARs for analysis of ‘in-house’ data. The ‘Training engine‘ makes appropriate corrections for systematic deviations produced by the baseline QSAR model based on analysis of similar compounds from the experimental data library. Expansion of this Self-training Library with user-defined experimental data for new compounds leads to instant improvement of prediction accuracy for the respective compound classes. Moreover, addition of 'in-house' data allows adapting the existing model to the particular experimental protocol used in your company and avoiding potential issues related to discrepancies between different experimental methods used for determination of drug interactions with P-gp.

If the compound is within model Applicability Domain (acceptable Reliability Index) accuracy and sensitivity of classification is close to 90% for both models.