Insilico docking studies of daidzeion compounds as selective estrogen receptor modulator (SERMS) breast cancer

Yani Suryani; Opik Taupiqurrohman; Ai Rikani; Epa Paujiah

doi:10.1051/matecconf/201819703009

All issues

Volume 197 (2018)

MATEC Web Conf., 197 (2018) 03009

Abstract

Open Access

Issue		MATEC Web Conf. Volume 197, 2018 The 3^rd Annual Applied Science and Engineering Conference (AASEC 2018)


Article Number		03009
Number of page(s)		5
Section		Computer Science
DOI		https://doi.org/10.1051/matecconf/201819703009
Published online		12 September 2018

MATEC Web of Conferences 197, 03009 (2018)

Insilico docking studies of daidzeion compounds as selective estrogen receptor modulator (SERMS) breast cancer

Yani Suryani¹^*, Opik Taupiqurrohman¹, Ai Rikani¹ and Epa Paujiah²

¹ UIN Sunan Gunung Djati Bandung, Department of Biology, 40614, West Java, Indonesia
² UIN Sunan Gunung Djati Bandung, Department of Biology Education, Bandung 40614, West Java, Indonesia

^* Corresponding author: yan_dhika@yahoo.com

Abstract

The aims of this study to analyze the potential of daidzein compounds as selective estrogen receptor modulators (SERMs) compared with 17-β estradiol. SERMs is a compound that can be used as a anticancer of breast cancer. The process of analysis is done computation, that is molecular docking. The research was conducted at Data Processing Laboratory of Department of Biology Faculty of Science and Technology, State Islamic University of Sunan Gunung Djati Bandung in December 2017 until February 2018. The result of analysis showed that daidzein compounds have excellent potential as SERMs. This is indicated by the very low energy value of binding affinity of Deidzein (-9.4 kcal / mol) compared to17-β estradiol (-8.9 kcal / mol). The smallest of energy binding affinity value indicates a very high binding ability.

This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Current usage metrics show cumulative count of Article Views (full-text article views including HTML views, PDF and ePub downloads, according to the available data) and Abstracts Views on Vision4Press platform.

Data correspond to usage on the plateform after 2015. The current usage metrics is available 48-96 hours after online publication and is updated daily on week days.

Initial download of the metrics may take a while.