Exploring the Role of Water Molecules in the Ligand Binding Domain of PDE4B and PDE4D: Virtual Screening Based Molecular Docking of Some Active Scaffolds
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Published:2019-07-01
Issue:4
Volume:15
Page:334-366
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ISSN:1573-4099
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Container-title:Current Computer-Aided Drug Design
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language:en
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Short-container-title:CAD
Author:
Singh Priya1, Mishra Mitali1, Agarwal Shivangi1, Sau Samaresh2, Iyer Arun K.2, Kashaw Sushil K.2
Affiliation:
1. Department of Pharmaceutical Sciences, Dr. Harisingh Gour University (A Central University), Sagar, MP, India 2. Use- inspired Biomaterials & Integrated Nano Delivery (U-BiND) Systems Laboratory, Department of Pharmaceutical Sciences, Wayne State University, Detroit, Michigan, MI, United States
Abstract
Background:
The phosphodiesterase (PDE) is a superfamily represented by four genes: PDE4A,
B,C, and D which cause the hydrolysis of phosphodiester bond of cAMP to yield inactive AMP. c-AMP
catalyzing enzyme is predominant in inflammatory and immunomodulatory cells. Therapy to treat Chronic
Obstructive Pulmonary Disease (COPD) with the use of PDE4 inhibitors is highly envisaged.
Objective:
A molecular docking experiment with large dataset of diverse scaffolds has been performed on
PDE4 inhibitors to analyze the role of amino acid responsible for binding and activation of the secondary
transmitters. Apart from the general docking experiment, the main focus was to discover the role of water
molecules present in the ligand-binding domain.
Methods:
All the compounds were docked in the PDE4B and PDE4D active cavity to produce the free
binding energy scores and spatial disposition/orientation of chemical groups of inhibitors around the cavity.
Under uniform condition, the experiments were carried out with and without water molecules in the LBD.
The exhaustive study was carried out on the Autodock 4.2 software and explored the role of water molecules
present in the binding domain.
Results:
In presence of water molecule, Roflumilast has more binding affinity (-8.48 Kcal/mol with
PDE4B enzyme and -8.91 Kcal/mol with PDE4D enzyme) and forms two hydrogen bonds with Gln443 and
Glu369 and amino acid with PDE4B and PDE4D enzymes respectively. While in absence of water molecule
its binding affinity has decreased (-7.3 Kcal/mol with PDE4B enzyme and -5.17 Kcal/mol with
PDE4D enzyme) as well as no H-bond interactions were observed. Similar observation was made with clinically
tested molecules.
Conclusion:
In protein-ligand binding interactions, appropriate selection of water molecules facilitated the
ligand binding, which eventually enhances the efficiency as well as the efficacy of ligand binding.
Publisher
Bentham Science Publishers Ltd.
Subject
Drug Discovery,Molecular Medicine,General Medicine
Reference32 articles.
1. Brown WM. Int J COPD, Treating COPD with PDE 4 inhibitors.,, 2007, 2,, 517-533, 2. Lee J, Lee H, Kim JA, Rhee CK. Int J COPD, Trend of cost and utilization of COPD medication in Korea.,, 2017, 12,, 27-33, 3. Fabbri LM, Hurd SS. Eur Respir J, Global strategy for the diagnosis, management and prevention of COPD: 2003 update.,, 2003, 22,, 1-, 4. Dhamane AD, Schwab P, Hopson S. Int J COPD, Association between adherence to medications for COPD and medications for other chronic conditions in COPD patients.,, 2017, 12,, 115-122, 5. Su Y, Long C, Yu Q, Zhang J, Wu D, Duan Z. Int J COPD, Global scientific collaboration in COPD research.,, 2017, 12,, 215-225,
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