Molecular docking studies for the identification of novel melatoninergic inhibitors for acetylserotonin-O-methyltransferase using different docking routines

Azam, Syed Sikander; Abbasi, Sumra Wajid

doi:10.1186/1742-4682-10-63

Cited by 168 publications

(86 citation statements)

References 39 publications

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“…It is a criterion for finding the distribution of atoms, molecules or other species around target specially interacting residues that are crucial for the stability of ligand during the ligand binding process [86]. Hydrogen bond interactions were calculated to check the stability of binding pocket residues (Arg215, Asn252, Asn279, His249…”

Section: Molecular Dynamics Simulationmentioning

confidence: 99%

Structural and dynamical aspects of Streptococcus gordonii FabH through molecular docking and MD simulations

Shamim

Abbasi

Azam

2015

Journal of Molecular Graphics and Modelling

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Section: Molecular Dynamics Simulationmentioning

confidence: 99%

Structural and dynamical aspects of Streptococcus gordonii FabH through molecular docking and MD simulations

Shamim

Abbasi

Azam

2015

Journal of Molecular Graphics and Modelling

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“…Thus, it will take some time for us to investigate the effects of lysoPC-22:4 on gastrointestinal tract transit in vivo. An increasing number of reports on virtual simulation have appeared in the literature [18][19][36][37]. In silico molecular docking studies have been used to support their pharmacological results.…”

Section: Pocketmentioning

confidence: 99%

Acute exposure to an electric field induces changes in human plasma lysophosphatidylcholine (lysoPC)-22:4 levels: Molecular insight into the docking of lysoPC-22:4 interaction with TRPV2

Nakagawa-Yagi¹,

Hara²,

Nakanishi³

et al. 2017

Integr Mol Med

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Medical treatment using high-voltage electric potential (HELP) devices to generate an electric field (EF) is an alternative therapy commonly used in Japan. However, the underlying mechanisms of the potential health benefits are not fully understood. To address this issue, we investigated the levels of lyso-form phospholipids using selected reaction monitoring (SRM) analysis in plasma samples obtained from healthy human subjects before and after a single HELP exposure (9 kV/electrode + 9 kV/electrode, 30 min). Lysophosphatidylcholine (lysoPC)-22:4 was significantly upregulated after HELP exposure. However, there was no effect on the levels of lysophosphatidic acid (lysoPA), or other lysoPC species. LysoPC is known to accelerate intestinal movement as a putative endogenous activator of transient receptor potential vanilloid 2 (TRPV2). We further examined the in silico docking simulation of lysoPC-22:4 with TRPV2. Docking results showed that lysoPC-22:4 has good binding energy (-8.2 kcal/mol). Our findings provide new insight into the molecular mechanisms of constipation alleviation by EF therapy.

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“…Molecular docking is an effective and competent tool playing an important and ever-increasing role in rational drug design. Docking is a computational procedure of searching for an appropriate ligand that fits both energetically and geometrically the protein's binding site [22].…”

Section: Dockingmentioning

confidence: 99%

“In Silico Metabolic Pathway Analysis and Docking Analysis of Treponema Pallidum Subs. Pallidum Nichols for Potential Drug Targets”

Mahendran

Jeyabasker

Manoharan

et al. 2017

Asian J Pharm Clin Res

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Objective: Syphilis is a sexually transmitted infection caused by the spirochaete, Treponema pallidum subspecies Pallidum nichols. In this study, a comparative metabolic pathway analysis and molecular docking were performed to identify putative drug targets. Methods:The biochemical pathways of T. pallidum subs. P. nichols and Homo sapiens were compared using kyoto encyclopedia of genes and genomes pathway(KEGG). The amino acid sequence of the selected enzymes were retrieved and Blastp was performed. Out of 9 enzymes, enolase was modeled using ModWeb, and the structure was validated using RAMPAGE. The active sites were identified using Metapocket 2.0 and further docked using AutoDock 4.2. Results:The enzymes which were not similar to that of H. sapiens were filtered out as potential drug targets. A total of 9 enzymes were retrieved which were present only in T. pallidum subs. P. nichols. The structure obtained from Homology modeling was validated using RAMPAGE which showed 96% of the residues in the favorable regions and 3% of the residues in the allowed region. Since the result obtained from RAMPAGE showed structural reliability further active sites were predicted. The docking analysis results showed the interaction between enolase and doxycycline. The atom H42 displayed in green has interacted with OD1 (Asp 317) with a distance of 1.9 Å depicts the best interaction and the structures were visualized using PyMol.Conclusion: Through this study, doxycycline which has antibacterial effect and a derivative of tetracycline could be one of the potential ligands against enolase.

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Molecular docking studies for the identification of novel melatoninergic inhibitors for acetylserotonin-O-methyltransferase using different docking routines

Cited by 168 publications

References 39 publications

Structural and dynamical aspects of Streptococcus gordonii FabH through molecular docking and MD simulations

Structural and dynamical aspects of Streptococcus gordonii FabH through molecular docking and MD simulations

Acute exposure to an electric field induces changes in human plasma lysophosphatidylcholine (lysoPC)-22:4 levels: Molecular insight into the docking of lysoPC-22:4 interaction with TRPV2

“In Silico Metabolic Pathway Analysis and Docking Analysis of Treponema Pallidum Subs. Pallidum Nichols for Potential Drug Targets”

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