Identification by Molecular Docking OfHomoisoflavones from Leopoldia Comosa As Ligands of Estrogen Receptors

Overview

Journal Molecules

Publisher MDPI

Specialty Biology

Date 2018 Apr 13

PMID 29649162

Citations 24

Authors

Fedora Grande

Bruno Rizzuti

Maria A Occhiuzzi

Giuseppina Ioele

Teresa Casacchia

Fabrizio Gelmini

Rita Guzzi

Antonio Garofalo

Giancarlo Statti

Affiliations

Soon will be listed here.

Abstract

The physiological responses to estrogen hormones are mediated within specific tissues by at least two distinct receptors, ER and ER. Several natural and synthetic molecules show activity by interacting with these proteins. In particular, a number of vegetal compounds known as phytoestrogens shows estrogenic or anti-estrogenic activity. The majority of these compounds belongs to the isoflavones family and the most representative one, genistein, shows anti-proliferative effects on various hormone-sensitive cancer cells, including breast, ovarian and prostate cancer. In this work we describe the identification of structurally related homoisoflavones isolated from (L.) Parl. (), a perennial bulbous plant, potentially useful as hormonal substitutes or complements in cancer treatments. Two of these compounds have been selected as potential ligands of estrogen receptors (ERs) and the interaction with both isoforms of estrogen receptors have been investigated through molecular docking on their crystallographic structures. The results provide evidence of the binding of these compounds to the target receptors and their interactions with key residues of the active sites of the two proteins, and thus they could represent suitable leads for the development of novel tools for the dissection of ER signaling and the development of new pharmacological treatments in hormone-sensitive cancers.

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