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DOI10.1093/toxsci/kfv168
Integrated Model of Chemical Perturbations of a Biological Pathway Using 18 In Vitro High-Throughput Screening Assays for the Estrogen Receptor
Judson, Richard S.1; Magpantay, Felicia Maria2; Chickarmane, Vijay3; Haskell, Cymra4; Tania, Nessy5; Taylor, Jean6; Xia, Menghang7; Huang, Ruili7; Rotroff, Daniel M.8,9; Filer, Dayne L.10; Houck, Keith A.1; Martin, Matthew T.1; Sipes, Nisha11; Richard, Ann M.1; Mansouri, Kamel10; Setzer, R. Woodrow1; Knudsen, Thomas B.1; Crofton, Kevin M.1; Thomas, Russell S.1
发表日期2015-11-01
ISSN1096-6080
卷号148期号:1页码:137-154
英文摘要

We demonstrate a computational network model that integrates 18 in vitro, high-throughput screening assays measuring estrogen receptor (ER) binding, dimerization, chromatin binding, transcriptional activation, and ER-dependent cell proliferation. The network model uses activity patterns across the in vitro assays to predict whether a chemical is an ER agonist or antagonist, or is otherwise influencing the assays through a manner dependent on the physics and chemistry of the technology platform ("assay interference"). The method is applied to a library of 1812 commercial and environmental chemicals, including 45 ER positive and negative reference chemicals. Among the reference chemicals, the network model correctly identified the agonists and antagonists with the exception of very weak compounds whose activity was outside the concentration range tested. The model agonist score also correlated with the expected potency class of the active reference chemicals. Of the 1812 chemicals evaluated, 111 (6.1%) were predicted to be strongly ER active in agonist or antagonist mode. This dataset and model were also used to begin a systematic investigation of assay interference. The most prominent cause of false-positive activity (activity in an assay that is likely not due to interaction of the chemical with ER) is cytotoxicity. The model provides the ability to prioritize a large set of important environmental chemicals with human exposure potential for additional in vivo endocrine testing. Finally, this model is generalizable to any molecular pathway for which there are multiple upstream and downstream assays available.


英文关键词estrogen receptor;EDSP;high-throughput screening;In vitro;prioritization;biological modeling
语种英语
WOS记录号WOS:000365547900013
来源期刊TOXICOLOGICAL SCIENCES
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/61760
作者单位1.US EPA, Res Triangle Pk, NC 27711 USA;
2.Univ Manitoba, Dept Math, Winnipeg, MB R3T 2N2, Canada;
3.CALTECH, Div Biol, Pasadena, CA 91125 USA;
4.Univ So Calif, Dept Math, Los Angeles, CA 90089 USA;
5.Smith Coll, Dept Math, Northampton, MA 01063 USA;
6.NYU, Courant Inst, New York, NY 10012 USA;
7.NIH, Chem Genom Ctr, Natl Ctr Adv Translat Sci, Rockville, MD 20892 USA;
8.N Carolina State Univ, Dept Stat, Raleigh, NC 27607 USA;
9.N Carolina State Univ, Bioinformat Res Ctr, Raleigh, NC 27607 USA;
10.US EPA, ORISE, Res Triangle Pk, NC 27711 USA;
11.NIH, Natl Toxicol Program, Res Triangle Pk, NC 27711 USA
推荐引用方式
GB/T 7714
Judson, Richard S.,Magpantay, Felicia Maria,Chickarmane, Vijay,et al. Integrated Model of Chemical Perturbations of a Biological Pathway Using 18 In Vitro High-Throughput Screening Assays for the Estrogen Receptor[J]. 美国环保署,2015,148(1):137-154.
APA Judson, Richard S..,Magpantay, Felicia Maria.,Chickarmane, Vijay.,Haskell, Cymra.,Tania, Nessy.,...&Thomas, Russell S..(2015).Integrated Model of Chemical Perturbations of a Biological Pathway Using 18 In Vitro High-Throughput Screening Assays for the Estrogen Receptor.TOXICOLOGICAL SCIENCES,148(1),137-154.
MLA Judson, Richard S.,et al."Integrated Model of Chemical Perturbations of a Biological Pathway Using 18 In Vitro High-Throughput Screening Assays for the Estrogen Receptor".TOXICOLOGICAL SCIENCES 148.1(2015):137-154.
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