In Silico Guidance for In Vitro Androgen and Glucocorticoid Receptor ToxCast Assays
Author(s) -
Timothy E. H. Allen,
Mark Nelms,
Stephen W. Edwards,
Jonathan M. Goodman,
Steve Gutsell,
Paul Russell
Publication year - 2020
Publication title -
environmental science and technology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.851
H-Index - 397
eISSN - 1520-5851
pISSN - 0013-936X
DOI - 10.1021/acs.est.0c01105
Subject(s) - in silico , computational biology , glucocorticoid receptor , androgen receptor , adverse outcome pathway , agonist , computational model , drug discovery , computer science , bioinformatics , biology , chemistry , receptor , biochemistry , artificial intelligence , genetics , prostate cancer , cancer , gene
Molecular initiating events (MIEs) are key events in adverse outcome pathways that link molecular chemistry to target biology. As they are based on chemistry, these interactions are excellent targets for computational chemistry approaches to in silico modeling. In this work, we aim to link ligand chemical structures to MIEs for androgen receptor (AR) and glucocorticoid receptor (GR) binding using ToxCast data. This has been done using an automated computational algorithm to perform maximal common substructure searches on chemical binders for each target from the ToxCast dataset. The models developed show a high level of accuracy, correctly assigning 87.20% of AR binders and 96.81% of GR binders in a 25% test set using holdout cross-validation. The 2D structural alerts developed can be used as in silico models to predict these MIEs and as guidance for in vitro ToxCast assays to confirm hits. These models can target such experimental work, reducing the number of assays to be performed to gain required toxicological insight. Development of these models has also allowed some structural alerts to be identified as predictors for agonist or antagonist behavior at the receptor target. This work represents a first step in using computational methods to guide and target experimental approaches.
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