Computational approach to identify potential antileishmanial activity of reported inhibitor, E5700 and two natural alkaloids against <i>Leishmania donovani</i> Squalene Synthase

Wadanambi, Padmika Madushanka

doi:10.1017/exp.2020.37

Cited by 2 publications

(6 citation statements)

References 12 publications

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“…In the top hit ligands, ancistrotanzanine B showed the best docking pose with the least binding energy (-9.83 kcal/mol and K i of 61.84 nM) with LdSQS closely followed by reported inhibitor 1 (E5700), ancistrotanzanine A, ancistrobenomine A, 5-epi-4 0 -O-demethylancistrobertsonine C, ancistroealaine B, ramiflorine B and 3-O-methyldiplacol with binding affinities of -9.81 kcal/ mol (Ki of 64.82 nM), -9.68 kcal/mol (K i of 80.37 nM), -9.54 kcal/mol (K i of 101.91 nM), -9.34 kcal/mol (K i of 143.41 nM), -9.32 kcal/mol (K i of 146.86 nM), -9.23 kcal/mol (K i of 171.07 nM) and -9.10 kcal/mol (K i of 213.00 nM) respectively. Interestingly, the docking scores for E5700 and ancistrotanzanine B in the current study, were slightly different than the previously published results where E5700 (-9.75 kcal/ mol) exhibited higher score than ancistrotanzanine B (-9.55 kcal/mol) [17].…”

Section: Grid Box Preparation and Virtual Screeningcontrasting

confidence: 99%

“…Based on the methodology followed in the previously published pilot study, 50 models of the LdSQS protein was built [ 17 ]. The solved crystal structure of LdSQS is not available at the RCSB Protein Data Bank ( https://www.rcsb.org/ ) [ 24 ].…”

Section: Methodsmentioning

confidence: 99%

“…Then the selected model was refined by quality information from MolProbity server [ 26 ] using UCSF Chimera v.1.12 [ 27 ]. The selected model was energy minimized up to 2100 steps by steepest descent algorithm in AMBER force field (using UCSF Chimera) instead of 1000 steps which were carried in the previous publication [ 17 ]. This additional step not only relieved steric clashes and improper contacts of the model but also that increased the values of validation results hence improving the quality of the model.…”

Section: Methodsmentioning

confidence: 99%

“…A pilot docking study using homology modeled LdSQS with the reported inhibitor (E5700) and two plant derived alkaloids (ancistrotanzanine b and holamine) was conducted and published by the first author [ 17 ]. The promising results from the pilot study led to design a full scale computational study to explore potent inhibitors from plant derived compounds against LdSQS.…”

Section: Introductionmentioning

confidence: 99%

“…In the current study, the modeled LdSQS protein was subjected to further energy minimization using steepest descent algorithm than in the previously published model [ 17 ]. This brought significant improvement in the ERRAT and MolProbity validation results of the modeled protein thus enhancing the accuracy of the new LdSQS model.…”

Section: Introductionmentioning

confidence: 99%

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Computational study to discover potent phytochemical inhibitors against drug target, squalene synthase from Leishmania donovani

Wadanambi¹,

Mannapperuma

2021

Heliyon

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Aims The parasite, Leishmania donovani is responsible for lethal visceral leishmaniasis (VL) in humans. There is a need to investigate novel medicines as antileishmanial drugs, as medication currently introduced for leishmaniasis may cause resistance, serious side-effects, chemical instability and high cost. Therefore, this computational study was designed to explore potential phytochemical inhibitors against Leishmania donovani squalene synthase (LdSQS) enzyme, a drug target. Main methods Multiple sequence alignment was carried to detect conserved regions across squalene synthases from different Leishmania spp. Their evolutionary relationships were studied by generating phylogenetic tree. Homology modeling method was used to build a three dimensional model of the protein. The validated model was explored by docking simulation with the phytochemicals of interest to identify the most potent inhibitors. Two reported inhibitors were used as references in the virtual screening. The top hit compounds (binding energy less than -9 kcal/mol) were further subjected to intermolecular interaction analysis, pharmacophore modeling, pharmacokinetic and toxicity prediction. Key findings Seven phytochemicals displayed binding energies less than -9 kcal/mol hence demonstrating ability to be strongly bound to the active site of LdSQS to inhibit the enzymatic activity. Ancistrotanzanine B demonstrated the lowest binding affinity of -9.83 kcal/mol superior to reported inhibitors in literature. Conserved two aspartate rich regions and two signatory motifs were found in the L. donovani squalene synthase by multiple sequence alignment. In addition, study of pharmacophore modeling confirmed that top hit phytochemicals and the reported inhibitor (E5700) share common chemical features for their biochemical interaction with LdSQS. Among seven phytochemicals, 3-O-methyldiplacol showed admissible physicochemical, pharmacokinetic and toxicity predictions compared to the reported inhibitors. All seven phytochemicals satisfied in silico prediction criteria for oral bioavailability. Significance Based on the current study, these hits can be further structurally optimized and validated under laboratory conditions to develop antileishmanial drugs.

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Section: Grid Box Preparation and Virtual Screeningcontrasting

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Computational study to discover potent phytochemical inhibitors against drug target, squalene synthase from Leishmania donovani

Wadanambi¹,

Mannapperuma

2021

Heliyon

Self Cite

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Antileishmanial Potential of Berberine Alkaloids From Berberis glaucocarpa Roots: Molecular Docking Suggests Relevant Leishmania Protein Targets

Alamzeb¹,

Ali²,

Mamoon-Ur-Rashid

et al. 2021

Natural Product Communications

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Leishmaniases are a spectrum of poverty-linked neglected parasitic diseases that are endemic in 88 countries around the globe and affect millions of people every year. Currently available chemotherapeutic options are inadequate due to side effects, high cost, prolonged treatment, and parasite resistance. Thus, there is an existing need to develop new potent and safer leishmanicidal drugs. Considering the folkloric antiulcer and leishmanicidal use of the genus Berberis and its alkaloids, 5 reported alkaloids, namely berberine (1), palmatine (2), columbamine (3), 8-trichloromethyldihydroberberine (4), and jatrorrhizine (5), were isolated from the roots of Berberis glaucocarpa using classical (column and preparative chromatography) and modern isolation techniques (Sephadex LH-20). Their structures were elucidated and established from 1D and 2D spectroscopic data. The isolated alkaloids displayed excellent antileishmanial potential with IC50 values ranging from 1.50 to 2.56 µM: 1 (1.50 ± 0.53 µM), 2 (2.31 ± 0.37 µM), 3 (2.56 ± 0.48 µM), 4 (1.40 ± 0.90 µM), 5 (2.44 ± 1.34 µM). While the IC50 value for the standard drug (Amphotericin-B) was found to be 1.08 ± 0.95 µM. All of the isolated alkaloids displayed excellent antileishmanial potential as well as minimal cytotoxicity against THP-1 monocytic cells. Molecular docking analysis has revealed Leishmania N-myristoyl transferase, methionyl-tRNA synthetase, pteridine reductase 1, oligopeptidase B, tyrosyl-tRNA synthetase, and/or glycerol-3-phosphate dehydrogenase to be potential protein targets for the alkaloids.

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Computational approach to identify potential antileishmanial activity of reported inhibitor, E5700 and two natural alkaloids against Leishmania donovani Squalene Synthase

Cited by 2 publications

References 12 publications

Computational study to discover potent phytochemical inhibitors against drug target, squalene synthase from Leishmania donovani

Computational study to discover potent phytochemical inhibitors against drug target, squalene synthase from Leishmania donovani

Antileishmanial Potential of Berberine Alkaloids From Berberis glaucocarpa Roots: Molecular Docking Suggests Relevant Leishmania Protein Targets

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