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DOI10.1289/EHP184
Evaluation of OASIS QSAR Models Using ToxCast (TM) in Vitro Estrogen and Androgen Receptor Binding Data and Application in an Integrated Endocrine Screening Approach
Bhhatarai, Barun1; Wilson, Daniel M.1; Price, Paul S.1; Marty, Sue1,2; Parks, Amanda K.1; Carney, Edward1
发表日期2016-09-01
ISSN0091-6765
卷号124期号:9页码:1453-1461
英文摘要

BACKGROUND: Integrative testing strategies (ITSs) for potential endocrine activity can use tiered in silico and in vitro models. Each component of an ITS should be thoroughly assessed.


OBJECTIVES: We used the data from three in vitro ToxCast (TM) binding assays to assess OASIS, a quantitative structure-activity relationship (QSAR) platform covering both estrogen receptor (ER) and androgen receptor (AR) binding. For stronger binders (described here as AC(50) < 1 mu M), we also examined the relationship of QSAR predictions of ER or AR binding to the results from 18 ER and 10 AR transactivation assays, 72 ER-binding reference compounds, and the in vivo uterotrophic assay.


METHODS: NovaScreen binding assay data for ER (human, bovine, and mouse) and AR (human, chimpanzee, and rat) were used to assess the sensitivity, specificity, concordance, and applicability domain of two OASIS QSAR models. The binding strength relative to the QSAR-predicted binding strength was examined for the ER data. The relationship of QSAR predictions of binding to transactivation- and pathway-based assays, as well as to in vivo uterotrophic responses, was examined.


RESULTS: The QSAR models had both high sensitivity (> 75%) and specificity (> 86%) for ER as well as both high sensitivity (92-100%) and specificity (70-81%) for AR. For compounds within the domains of the ER and AR QSAR models that bound with AC(50) < 1 mu M, the QSAR models accurately predicted the binding for the parent compounds. The parent compounds were active in all transactivation assays where metabolism was incorporated and, except for those compounds known to require metabolism to manifest activity, all assay platforms where metabolism was not incorporated. Compounds in-domain and predicted to bind by the ER QSAR model that were positive in ToxCast (TM) ER binding at AC(50) < 1 mu M were active in the uterotrophic assay.


CONCLUSIONS: We used the extensive ToxCast (TM) HTS binding data set to show that OASIS ER and AR QSAR models had high sensitivity and specificity when compounds were in-domain of the models. Based on this research, we recommend a tiered screening approach wherein a) QSAR is used to identify compounds in-domain of the ER or AR binding models and predicted to bind; b) those compounds are screened in vitro to assess binding potency; and c) the stronger binders (AC(50) < 1 mu M) are screened in vivo. This scheme prioritizes compounds for integrative testing and risk assessment. Importantly, compounds that are not in-domain, that are predicted either not to bind or to bind weakly, that are not active in in vitro, that require metabolism to manifest activity, or for which in vivo AR testing is in order, need to be assessed differently.


语种英语
WOS记录号WOS:000382530200026
来源期刊ENVIRONMENTAL HEALTH PERSPECTIVES
来源机构美国环保署
文献类型期刊论文
条目标识符http://gcip.llas.ac.cn/handle/2XKMVOVA/57469
作者单位1.Dow Chem Co USA, Toxicol Environm Res & Consulting, Midland, MI 48674 USA;
2.US EPA, Natl Exposure Res Lab, Res Triangle Pk, NC 27711 USA
推荐引用方式
GB/T 7714
Bhhatarai, Barun,Wilson, Daniel M.,Price, Paul S.,et al. Evaluation of OASIS QSAR Models Using ToxCast (TM) in Vitro Estrogen and Androgen Receptor Binding Data and Application in an Integrated Endocrine Screening Approach[J]. 美国环保署,2016,124(9):1453-1461.
APA Bhhatarai, Barun,Wilson, Daniel M.,Price, Paul S.,Marty, Sue,Parks, Amanda K.,&Carney, Edward.(2016).Evaluation of OASIS QSAR Models Using ToxCast (TM) in Vitro Estrogen and Androgen Receptor Binding Data and Application in an Integrated Endocrine Screening Approach.ENVIRONMENTAL HEALTH PERSPECTIVES,124(9),1453-1461.
MLA Bhhatarai, Barun,et al."Evaluation of OASIS QSAR Models Using ToxCast (TM) in Vitro Estrogen and Androgen Receptor Binding Data and Application in an Integrated Endocrine Screening Approach".ENVIRONMENTAL HEALTH PERSPECTIVES 124.9(2016):1453-1461.
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