Abstract
The ABCB1 transporter also known as P-glycoprotein (P-gp) is a transmembrane protein belonging to the ATP binding cassette super-family of transporters; it is a xenobiotic efflux pump that limits intracellular drug accumulation by pumping the compounds out of cells. P-gp contributes to a decrease of toxicity and possesses broad substrate specificity. It is involved in the failure of numerous anticancer and antiviral chemotherapies due to the multidrug resistance (MDR) phenomenon, where it removes the chemotherapeutics out of the targeted cells. Understanding the details of the ligand–P-gp interaction is therefore crucial for the development of drugs that might overcome the MRD phenomenon and for obtaining a more effective prediction of the toxicity of certain compounds. In this work, an in silico modeling was performed using homology modeling and molecular docking methods with the aim of better understanding the ligand–P-gp interactions. Based on different mouse P-gp structural templates from the PDB repository, a 3D model of the human P-gp (hP-gp) was constructed by means of protein homology modeling. The homology model was then used to perform molecular docking calculations on a set of thirteen compounds, including some well-known compounds that interact with P-gp as substrates, inhibitors, or both. The sum of ranking differences (SRD) was employed for the comparison of the different scoring functions used in the docking calculations. A consensus-ranking scheme was employed for the selection of the top-ranked pose for each docked ligand. The docking results showed that a high number of π interactions, mainly π–sigma, π–alkyl, and π–π type of interactions, together with the simultaneous presence of hydrogen bond interactions contribute to the stability of the ligand–protein complex in the binding site. It was also observed that some interacting residues in hP-gp are the same when compared to those observed in a co-crystallized ligand (PBDE-100) with mouse P-gp (PDB ID: 4XWK). Our in silico approach is consistent with available experimental results regarding P-gp efflux transport assay; therefore it could be useful in the prediction of the role of new compounds in systemic toxicity.
Highlights
The ATP-binding cassette (ABC) transporter ABCB1, known as P-glycoprotein (P-gp) is a transmembrane efflux transporter with a broad substrate specificity that limits intracellular drug accumulation and contributes to a decrease of toxicity
We developed a human P-gp (hP-gp) homology model based on mouse P-gp (mP-gp) multiple templates that can be used in further docking simulations
The results demonstrated a small Main-chain root mean square deviation (RMSD) against the crystal structure of mP-gp (PDB ID: 4M1M) with values of 0.24 Å and 0.70 Å for SWISS-MODEL and I-TASSER models, respectively
Summary
The ATP-binding cassette (ABC) transporter ABCB1, known as P-glycoprotein (P-gp) is a transmembrane efflux transporter with a broad substrate specificity that limits intracellular drug accumulation and contributes to a decrease of toxicity. The structure quality assessment made using the online tools PROCHECK, Verify 3D, ERRAT, and PROVE suggested that the three hP-gp models developed are as good as the crystal structure of the mP-gp (PDB ID: 4M1M) used as a template. They are reliable and of suitable quality for further molecular docking simulations. ERRAT and PROVE scores as well as PROCHECK assessments (Figure S6) suggest that truncated hP-gp model (without NBDs) is highly comparable to the selected one in terms of quality and reliability, allowing the use of the selected full-length I-TASSER hP-gp model for further structure-based (molecular docking calculations)
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