In Silico Based Approach to Investigate Plant Lignans as inhibitor Candidates for Estrogen Receptor in Breast Cancer

Background: In the last decades, growing evidence demonstrates interest in phytoestrogen intake to modulate targets in different types of cancer. Plant lignans have proven efficacious in blocking estrogen receptors of breast cancer cells. Among them, four phytoestrogen lignans: pinoresinol, matairesinol, lariciresinol, and secoisolariciresinol have been most studied. However, available studies have mostly dealt with anti-cancer effects of groups of lignans in certain foods or plants and the effects of specific lignans, especially from a molecular interaction viewpoint, have been rarely addressed in the literature. Objective: We aimed to in silico predict pharmacological properties, binding ability and binding strength of pinoresinol, matairesinol, lariciresinol and secoisolariciresinol as possible inhibitors of estrogen receptor alpha which is the most important biomarker in breast cancer. Methods: Firstly, we evaluated the pharmacological properties of four lignans using SwissADME. Then we investigated the ligand-receptor interactions of these molecules as positively appraised ligands for ER-positive breast cancer targeted therapy using docking method. We finally compared the inhibitory effect possibility of the lignans against endoxifen which is the active metabolite of tamoxifen. Results: The best binding affinity of endoxifen, matairesinol, pinoresinol, lariciresinol and secoisolariciresinol were respectively -9.2, -7.5, -6.7, -6.7, -5.8 kcal/mol. In the meantime, matairesinol showed the minimum binding energy than other studied lignans in addition to the most similar interactions to endoxifen with conserved domain residues of the active site pocket in Leu:391, Ala:350, Met:421, and Phe:404. Conclusion: Among the studied lignans, matairesinol showed the favorable pharmacokinetics and drug-likeliness properties, the least binding energy as well as the most common interactions in conserved residues of the active site pocket with estrogens. This makes it a molecule with low number of nonspecific interactions, better target selectivity, and hence fewer side effects. Thus, our results introduce matairesinol as a possibly effective anti-estrogen receptor inhibitor candidate.

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In silico study of curcumol, curcumenol, isocurcumenol, and β-sitosterol as potential inhibitors of estrogen receptor alpha of breast cancer

Medical Journal of Indonesia ◽

10.13181/mji.v23i1.684 ◽

2014 ◽

pp. 15 ◽

Cited By ~ 2

Author(s):

Resmi Mustarichiei ◽

Jutti Levitas ◽

Jopi Arpina

Keyword(s):

Breast Cancer ◽

Estrogen Receptor ◽

In Silico ◽

Estrogen Receptor Alpha ◽

Receptor Alpha ◽

In Silico Study ◽

Potential Inhibitors

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In silico approach for revealing the anti-breast cancer and estrogen receptor alpha inhibitory activity of Artocarpus altilis

10.1063/1.5062801 ◽

2018 ◽

Author(s):

Aida Fitriah ◽

Kholifah Holil ◽

Umaiyatus Syarifah ◽

Fitriyah ◽

Didik Huswo Utomo

Keyword(s):

Breast Cancer ◽

Estrogen Receptor ◽

Inhibitory Activity ◽

In Silico ◽

Estrogen Receptor Alpha ◽

Artocarpus Altilis ◽

Receptor Alpha

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Computer-Aided Drug Repurposing: A Cyclooxygenase-2 Inhibitor Celecoxib as a Ligand for Estrogen Receptor Alpha

Indonesian Journal of Chemistry ◽

10.22146/ijc.21196 ◽

2015 ◽

Vol 15 (3) ◽

pp. 274-280 ◽

Cited By ~ 3

Author(s):

Enade Perdana Istyastono ◽

Florentinus Dika Octa Riswanto ◽

Sri Hartati Yuliani

Keyword(s):

Breast Cancer ◽

Estrogen Receptor ◽

In Silico ◽

Estrogen Receptor Alpha ◽

Cyclooxygenase 2 ◽

Cytotoxic Activities ◽

In Vitro Test ◽

Receptor Alpha ◽

Vitro Test

A cyclooxygenase-2 (COX-2) inhibitor celecoxib has been previously reported to have cytotoxic activities towards gastric, prostate, ovarian, colon and breast cancer cell lines. This article reports that the cytotoxic activities of celecoxib could be resulted from its activity as a potent ligand for estrogen receptor alpha (ERα). Aided by molecular docking simulations, an in silico test to examine whether celecoxib is a ligand for estrogen receptor alpha (ERα) was performed followed by in vitro test employing cytotoxic assay using 3-[4,5-dimethylthiazol-2-yl]-2,5-diphenyltetrazolium bromide (MTT) method. The compound was extracted from Celebrex®. Measured by using UV spectrophotometric method at 255.5 nm, it was identified that the content of celecoxib was 102.15 mg/271.48 mg capsule content. The in silico test indicated that celecoxib is a potent ligand for ERα. This finding was confirmed experimentally by an in vitro test that celecoxib has a comparable activity as an ERα ligand to tamoxifen, a drug of choice for breast cancer treatment.

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In silico Molecular Modelling of Selected Natural Ligands and their Binding Features with Estrogen Receptor Alpha

Current Computer - Aided Drug Design ◽

10.2174/1573409914666181008165356 ◽

2018 ◽

Vol 15 (1) ◽

pp. 89-96 ◽

Cited By ~ 5

Author(s):

V.L. Maruthanila ◽

R. Elancheran ◽

Nand Kishor Roy ◽

Anupam Bhattacharya ◽

Ajaikumar B. Kunnumakkara ◽

...

Keyword(s):

Breast Cancer ◽

Estrogen Receptor ◽

Cell Line ◽

In Silico ◽

Estrogen Receptor Alpha ◽

Natural Compounds ◽

Pharmacokinetic Parameters ◽

Anticancer Activities ◽

Receptor Alpha ◽

Mcf 7

Background: Breast cancer is one of the most common cancers diagnosed among women. It is now recognized that two receptors mediate estrogen action and the presence of estrogen receptor alpha (ERα) correlates with better prognosis and the likelihood of response to hormonal therapy. ERα is an attractive target for the treatment of breast cancer. Most of the drugs currently used for the breast cancer treatment have numerous side effects and they are often unsuccessful in removing the tumour completely. Hence, we focused on natural compounds like flavonoids, polyphenols, etc. which do not exhibit any high toxic effects against normal cells. </P><P> Objectives: To identify the potential natural inhibitors for BCa through an optimised in silico approach. </P><P> Methods: Structural modification and molecular docking-based screening approaches were imposed to identify the novel natural compounds by using Schrödinger (Maestro 9.5). The Qikprop v3.5 was used for the evaluation of important ADME parameters and its permissible ranges. Cytotoxicity of the compounds was evaluated by MTT assay against MCF-7 Cell lines. Results: From the docking studies, we found that the compounds, Myricetin, Quercetin, Apigenin, Luteolin and Baicalein showed the highest Glide Scores -10.78, -9.48, -8.92, -8.87 and -8.82 kcal mol-1 respectively. Of these, Luteolin and Baicalein showed the significant IC50 values (25 ± 4.0 and 58.3 ± 4.4 µM, respectively) against MCF-7 cell line. The ADME profiling of the test compounds was evaluated to find the drug-likeness and pharmacokinetic parameters. We mainly focused on in silico study to dock the compounds into the human estrogen receptor ligand binding domain (hERLBD) and compare their predicted binding affinity with known antiestrogens. Myricetin, Quercetin, Apigenin, Luteolin and Baicalein were identified as the most promising among all. Of these, Luteolin and Baicalein showed significant anticancer activities against MCF-7 cell line. These findings may provide basic information for the development of anti-breast cancer agents.

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