Identification of putative estrogen receptor-mediated endocrine disrupting chemicals using QSAR- and structure-based virtual screening approaches

Zhang, Liying; Sedykh, Alexander; Tripathi, Ashutosh; Zhu, Hao; Afantitis, Antreas; Mouchlis, Varnavas D.; Melagraki, Georgia; Rusyn, Ivan; Tropsha, Alexander

doi:10.1016/j.taap.2013.04.032

Cited by 80 publications

(52 citation statements)

References 44 publications

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“…This is in agreement with earlier studies showing that non-linear methods (especially k-NN which is implemented within the ASNN method) result in the highest prediction accuracy for E-, A-, and T-binding Gramatica, 2010b, 2010a;Papa et al, 2013). Obtained statistics for the EAT models with highest balanced accuracy corresponded or were slightly higher than for recently published models using similar data (Li and Gramatica, 2010b;Jensen et al, 2011;Papa et al, 2013;Zhang et al, 2013). The ASNN models are, however, difficult to interpret and thus as suggested by Vorberg and Tetko (2014), PLS models were used to increase our understanding on fundamental structural characteristics of EAT binders and non-binders.…”

Section: Development Of Eat Modelssupporting

confidence: 91%

“…Many of these models can be applied only to a limited number of compounds. Models with relatively wide applicability have been developed for predicting binding affinity to the estrogen Serafimova et al, 2007;Li and Gramatica, 2010b;Toropov et al, 2012;Yi and Zhang, 2012;Zhang et al, 2013) and androgen receptors Li et al, 2009Li et al, , 2013aLi and Gramatica, 2010a;Jensen et al, 2011;Todorov et al, 2011). To our knowledge, studies on the use of QSAR models for prioritizing potential endocrine disruptors considering multiple endpoints were limited to two mechanisms of action (Li and Gramatica, 2010b) or to one group of compounds sharing similar structural features (Juberg et al, 2013), for example brominated flame retardants (Kovarich et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

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Identifying potential endocrine disruptors among industrial chemicals and their metabolites – development and evaluation of in silico tools

et al. 2015

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The aim of this study was to improve the identification of endocrine disrupting chemicals (EDCs) by developing and evaluating in silico tools that predict interactions at the estrogen (E) and androgen (A) receptors, and binding to transthyretin (T). In particular, the study focuses on evaluating the use of the EAT models in combination with a metabolism simulator to study the significance of bioactivation for endocrine disruption. Balanced accuracies of the EAT models ranged from 77-87%, 62-77%, and 65-89% for E-, A-, and T-binding respectively. The developed models were applied on a set of more than 6000 commonly used industrial chemicals of which 9% were predicted E- and/or A-binders and 1% were predicted T-binders. The numbers of E- and T-binders increased 2- and 3-fold, respectively, after metabolic transformation, while the number of A-binders marginally changed. In-depth validation confirmed that several of the predicted bioactivated E- or T-binders demonstrated in vivo estrogenic activity or influenced blood levels of thyroxine in vivo. The metabolite simulator was evaluated using in vivo data from the literature which showed a 50% accuracy for studied chemicals. The study stresses, in summary, the importance of including metabolic activation in prioritization activities of potentially emerging contaminants.

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Section: Development Of Eat Modelssupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Identifying potential endocrine disruptors among industrial chemicals and their metabolites – development and evaluation of in silico tools

et al. 2015

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“…All four possible ER classes were considered: ER-α bound to agonist, ER-α bound to antagonist, ER-β bound to agonist and ER-β bound to antagonist. For each of these, two crystal structures were retrieved from PDB: one previously considered by Zhang et al [28] for the identification of new EDs based on docking simulations, and the other recently selected by Kolšek et al [17] based on their capability to provide highly predictive docking-based classification models. On the other hand, the choice of eight different x-ray solved crystals (comprising ER-α and ER-β complexes for agonists and antagonists) was made to possibly cover a broader spectrum of possible biological actions of compounds comprised within the EPA training dataset.…”

Section: Molecular Dockingmentioning

confidence: 99%

Docking-Based Classification Models for Exploratory Toxicology Studies on High-Quality Estrogenic Experimental Data

et al. 2015

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“…The proper application of this technique can develop molecules with optimistic efficacy. Keeping in mind the objective of immense utility of SERMs for the treatment of post-menopausal diseases, researchers in academia as well as in industry are dedicated to the development of synthetic therapeutic SERMs for estrogen therapy (Brogia et al 2013;Chang et al 2013;Lewis et al 1995;Mukherjee et al 2005;Smith et al 2007;Zhang et al 2013). …”

Section: Introductionmentioning

confidence: 99%

Identification of structural requirements of estrogen receptor modulators using pharmacoinformatics techniques for application to estrogen therapy

et al. 2016

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An attempt was made in the present study to explore the structural requirements of known estrogen receptor (ER) modulators for biological activity using pharmacoinformatics approaches to elucidate critical functionalities for new, potent and less toxic chemical agents for successful application in estrogen therapy. For this purpose a group of non-steroidal ligands, 7-thiabicyclo[2.2.1]hept-2-ene-7-oxide derivatives were collected from the literature to perform quantitative structure-activity relationship (QSAR), pharmacophore and molecular docking studies. The 2D QSAR models (R for α-and β-subtypes respectively. The functionalities developed in the QSAR and pharmacophore studies were substantiated by molecular docking which provided the preferred orientation of ligands for effective interaction at the active site cavity.

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Identification of putative estrogen receptor-mediated endocrine disrupting chemicals using QSAR- and structure-based virtual screening approaches

Cited by 80 publications

References 44 publications

Identifying potential endocrine disruptors among industrial chemicals and their metabolites – development and evaluation of in silico tools

Identifying potential endocrine disruptors among industrial chemicals and their metabolites – development and evaluation of in silico tools

Docking-Based Classification Models for Exploratory Toxicology Studies on High-Quality Estrogenic Experimental Data

Identification of structural requirements of estrogen receptor modulators using pharmacoinformatics techniques for application to estrogen therapy

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