Determinative factors in inhibition of aquaporin by different pharmaceuticals: Atomic scale overview by molecular dynamics simulation |
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| Authors: | Vahid Fadaei Naeini Masumeh Foroutan Mina Maddah Yves Rémond Majid Baniassadi |
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| Affiliation: | 1. School of Mechanical Engineering, College of Engineering, University of Tehran, Tehran, Iran;2. Department of Physical Chemistry, School of Chemistry, College of Science, University of Tehran, Tehran, Iran;3. University of Strasbourg, ICube laboratory/CNRS, 2 Rue Boussingault, 67000 Strasbourg, France |
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| Abstract: | The inhibition of water permeation through aquaporins by ligands of pharmaceutical compounds is considered as a method to control the cell lifetime. The inhibition of aquaporin 1 (AQP1) by bacopaside-I and torsemide, was explored and its atomistic nature was elucidated by molecular docking and molecular dynamics (MD) simulation collectively along with Poisson-Boltzmann surface area (PBSA) method. Docking results revealed that torsemide has a lower level of docking energy in comparison with bacopaside-I at the cytoplasmic side. Furthermore, the effect of steric constraints on water permeation was accentuated. Bacopaside-I inhibits the channel properly due to the strong interaction with the channel and larger spatial volume, whereas torsemide blocks the cytoplasmic side of the channel imperfectly. The most probable active sites of AQP1 for the formation of hydrogen bonds between the inhibitor and the channel were identified by numerical analysis of the bonds. Eventually, free energy assessments indicate that binding of both inhibitors is favorable in complex with AQP1, and van der Waals interaction has an important contribution in stabilizing the complexes. |
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| Keywords: | Aquaporin Inhibition Bacopaside-I Torsemide Binding free energy Molecular docking Molecular dynamics simulation |
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