AI Article Synopsis
- Molecular docking and DFT simulations were used to explore how cyclodextrins (α-CD, β-CD, γ-CD) interact with the P-glycoprotein (P-gp), which plays a significant role in drug resistance, especially in cancer treatment and neurological disorders.
- The study focused on understanding the docking mechanism between cyclodextrins and P-gp, emphasizing hydrophobic and electrostatic interactions that could impact drug delivery across the blood-brain barrier.
- The results suggest that these interactions could help in designing new nanotherapeutic drugs to overcome drug resistance, ultimately improving treatment outcomes.
Article Abstract
Background: Herein, molecular docking approaches and DFT ab initio simulations were combined for the first time, to study the key interactions of cyclodextrins (CDs: α-CD, β-CD, and γ-CD) family with potential pharmacological relevance and the multidrug resistance P-gp protein toward efficient drug-delivery applications. The treatment of neurological disorders and cancer therapy where the multiple drug-resistance phenomenon mediated by the P-gp protein constitutes the fundamental cause of unsuccessful therapies.
Objectives: To understand more about the CD docking mechanism and the P-gp.
Methods: In order to achieve the main goal, the computational docking process was used. The observed docking-mechanism of the CDs on the P-gp was fundamentally based on hybrid backbone/side-chain hydrophobic interactions,and also hybrid electrostatic/side-chain interactions of the CD-ligands' OHmotifs with acceptor and donor characteristics, which might theoretically cause local perturbations in the TMD/P-gp inter-residues network, influencing ligand extrusion through the blood-brain barrier. P-gp residues were conformationally favored. Despite the structural differences, all the cyclodextrins exhibit very close Gibbs free binding energy values (or affinity) by the P-gp binding site (transmembrane domains - TMDs).
Result: The obtained theoretical docking-mechanism of the CDs on the P-gp was fundamentally based on hybrid backbone/side-chain hydrophobic interactions, and also hybrid electrostatic/side-chain interactions of the OH-motifs of the CD-ligands with acceptor and donor properties which theoretically could induce allosteric local-perturbations in the TMDs-inter-residues network of P-gp modulating to the CD-ligand extrusion from the blood-brain-barrier (or cancer cells).
Conclusion: Finally, these theoretical results open new horizons for evaluating new nanotherapeutic drugs with potential pharmacological relevance for efficient drug-delivery applications and precision nanomedicine.
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| http://dx.doi.org/10.2174/1568026622666220303115102 | DOI Listing |
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