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Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)

Molecular docking was done to assess the binding affinity of 6-paradol (6PRD), Zingerone (ZGR) and Zerumbone (ZRB) ligand-ERα complex in comparison to Hydroxytamoxifen (HTMX). Docking results showed that Glu353 and Arg394 active residues forms hydrogen bonding with 6PRD and ZGR. Glu353, Leu387 and A...

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Main Authors: Sharif, Faez, Azirudin, Athirah, Saedudin, RD Rohmat, Mohd Yunus, Afdzal, Abdul Hamid, Azzmer Azzar, Kasim, Shahreen
Format: Article
Language:English
Published: Penerbit UTHM 2018
Subjects:
TP248.13-248.65 Biotechnology
Online Access:http://eprints.uthm.edu.my/3644/1/AJ%202018%20%28706%29%20Molecular%20docking%20analysis%20of%206-paradol%2C%20zingerone%20and%20zerumbone%20against%20human%20Estrogen%20Receptor%20Alpha%20%28ER%C9%91%29.pdf
http://eprints.uthm.edu.my/3644/
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spelling my.uthm.eprints.36442021-11-21T04:44:25Z http://eprints.uthm.edu.my/3644/ Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ) Sharif, Faez Azirudin, Athirah Saedudin, RD Rohmat Mohd Yunus, Afdzal Abdul Hamid, Azzmer Azzar Kasim, Shahreen TP248.13-248.65 Biotechnology Molecular docking was done to assess the binding affinity of 6-paradol (6PRD), Zingerone (ZGR) and Zerumbone (ZRB) ligand-ERα complex in comparison to Hydroxytamoxifen (HTMX). Docking results showed that Glu353 and Arg394 active residues forms hydrogen bonding with 6PRD and ZGR. Glu353, Leu387 and Arg394 were the three identical residues found to formed hydrophobic interaction in HTMX-ERα, 6PRD-ERα and ZGR-ERα. HTMX showed lowest binding energy (-10.71 ± 0.43 kcal/mol) followed by ZRB (-8.66 ± 0.04 kcal/mol), 6PRD (-6.92 ± 0.14 kcal/mol) and ZGR (-5.93 ± 0.31 kcal/mol). Inhibition constant (Ki) range of 6PRD-ERα was found to be drastically lower than HTMX-ERα, ZGR-ERα and ZRB-ERα. Based on the docking analysis, the three bioactive compounds were showed to poses low potential as substitute towards tamoxifen. Future study is recommended for analysing 6PRD potential in substituting estradiol as Hormone Replacement Therapy (HRT) for breast cancer. Penerbit UTHM 2018 Article PeerReviewed text en http://eprints.uthm.edu.my/3644/1/AJ%202018%20%28706%29%20Molecular%20docking%20analysis%20of%206-paradol%2C%20zingerone%20and%20zerumbone%20against%20human%20Estrogen%20Receptor%20Alpha%20%28ER%C9%91%29.pdf Sharif, Faez and Azirudin, Athirah and Saedudin, RD Rohmat and Mohd Yunus, Afdzal and Abdul Hamid, Azzmer Azzar and Kasim, Shahreen (2018) Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ). International Journal of Integrated Engineering, 10 (6). pp. 113-118. ISSN 2229-838X
institution Universiti Tun Hussein Onn Malaysia
building UTHM Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Tun Hussein Onn Malaysia
content_source UTHM Institutional Repository
url_provider http://eprints.uthm.edu.my/
language English
topic TP248.13-248.65 Biotechnology
spellingShingle TP248.13-248.65 Biotechnology
Sharif, Faez
Azirudin, Athirah
Saedudin, RD Rohmat
Mohd Yunus, Afdzal
Abdul Hamid, Azzmer Azzar
Kasim, Shahreen
Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)
description Molecular docking was done to assess the binding affinity of 6-paradol (6PRD), Zingerone (ZGR) and Zerumbone (ZRB) ligand-ERα complex in comparison to Hydroxytamoxifen (HTMX). Docking results showed that Glu353 and Arg394 active residues forms hydrogen bonding with 6PRD and ZGR. Glu353, Leu387 and Arg394 were the three identical residues found to formed hydrophobic interaction in HTMX-ERα, 6PRD-ERα and ZGR-ERα. HTMX showed lowest binding energy (-10.71 ± 0.43 kcal/mol) followed by ZRB (-8.66 ± 0.04 kcal/mol), 6PRD (-6.92 ± 0.14 kcal/mol) and ZGR (-5.93 ± 0.31 kcal/mol). Inhibition constant (Ki) range of 6PRD-ERα was found to be drastically lower than HTMX-ERα, ZGR-ERα and ZRB-ERα. Based on the docking analysis, the three bioactive compounds were showed to poses low potential as substitute towards tamoxifen. Future study is recommended for analysing 6PRD potential in substituting estradiol as Hormone Replacement Therapy (HRT) for breast cancer.
format Article
author Sharif, Faez
Azirudin, Athirah
Saedudin, RD Rohmat
Mohd Yunus, Afdzal
Abdul Hamid, Azzmer Azzar
Kasim, Shahreen
author_facet Sharif, Faez
Azirudin, Athirah
Saedudin, RD Rohmat
Mohd Yunus, Afdzal
Abdul Hamid, Azzmer Azzar
Kasim, Shahreen
author_sort Sharif, Faez
title Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)
title_short Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)
title_full Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)
title_fullStr Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)
title_full_unstemmed Molecular docking analysis of 6-paradol, zingerone and zerumbone against human Estrogen Receptor Alpha (ERɑ)
title_sort molecular docking analysis of 6-paradol, zingerone and zerumbone against human estrogen receptor alpha (erɑ)
publisher Penerbit UTHM
publishDate 2018
url http://eprints.uthm.edu.my/3644/1/AJ%202018%20%28706%29%20Molecular%20docking%20analysis%20of%206-paradol%2C%20zingerone%20and%20zerumbone%20against%20human%20Estrogen%20Receptor%20Alpha%20%28ER%C9%91%29.pdf
http://eprints.uthm.edu.my/3644/
_version_ 1738581150230642688
score 13.160551

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