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DOI10.1289/ehp.1510385
Systems Toxicology of Male Reproductive Development: Profiling 774 Chemicals for Molecular Targets and Adverse Outcomes
Leung, Maxwell C. K.1,2; Phuong, Jimmy2; Baker, Nancy C.3; Sipes, Nisha S.1,2; Klinefelter, Gary R.4; Martin, Matthew T.2; McLaurin, Keith W.1,2; Setzer, R. Woodrow2; Darney, Sally Perreault4,5; Judson, Richard S.2; Knudsen, Thomas B.2
发表日期2016-07-01
ISSN0091-6765
卷号124期号:7页码:1050-1061
英文摘要

BACKGROUND: Trends in male reproductive health have been reported for increased rates of testicular germ cell tumors, low semen quality, cryptorchidism, and hypospadias, which have been associated with prenatal environmental chemical exposure based on human and animal studies.


OBJECTIVE: In the present study we aimed to identify significant correlations between environmental chemicals, molecular targets, and adverse outcomes across a broad chemical landscape with emphasis on developmental toxicity of the male reproductive system.


METHODS: We used U.S. EPA's animal study database (ToxRefDB) and a comprehensive literature analysis to identify 774 chemicals that have been evaluated for adverse effects on male reproductive parameters, and then used U.S. EPA's in vitro high-throughput screening (HTS) database (ToxCastDB) to profile their bioactivity across approximately 800 molecular and cellular features.


RESULTS: A phenotypic hierarchy of testicular atrophy, sperm effects, tumors, and malformations, a composite resembling the human testicular dysgenesis syndrome (TDS) hypothesis, was observed in 281 chemicals. A subset of 54 chemicals with male developmental consequences had in vitro bioactivity on molecular targets that could be condensed into 156 gene annotations in a bipartite network.


CONCLUSION: Computational modeling of available in vivo and in vitro data for chemicals that produce adverse effects on male reproductive end points revealed a phenotypic hierarchy across animal studies consistent with the human TDS hypothesis. We confirmed the known role of estrogen and androgen signaling pathways in rodent TDS, and importantly, broadened the list of molecular targets to include retinoic acid signaling, vascular remodeling proteins, G-protein coupled receptors (GPCRs), and cytochrome P450s.


语种英语
WOS记录号WOS:000380749300028
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/60719
作者单位1.Oak Ridge Inst Sci & Educ, Oak Ridge, TN USA;
2.US EPA, Natl Ctr Computat Toxicol, Res Triangle Pk, NC 27711 USA;
3.Lockheed Martin, Res Triangle Pk, NC USA;
4.US EPA, Natl Hlth & Environm Effects Res Lab, Res Triangle Pk, NC 27711 USA;
5.NIEHS, Environm Hlth Perspect, NIH, US Dept HHS, POB 12233, Res Triangle Pk, NC 27709 USA
推荐引用方式
GB/T 7714
Leung, Maxwell C. K.,Phuong, Jimmy,Baker, Nancy C.,et al. Systems Toxicology of Male Reproductive Development: Profiling 774 Chemicals for Molecular Targets and Adverse Outcomes[J]. 美国环保署,2016,124(7):1050-1061.
APA Leung, Maxwell C. K..,Phuong, Jimmy.,Baker, Nancy C..,Sipes, Nisha S..,Klinefelter, Gary R..,...&Knudsen, Thomas B..(2016).Systems Toxicology of Male Reproductive Development: Profiling 774 Chemicals for Molecular Targets and Adverse Outcomes.ENVIRONMENTAL HEALTH PERSPECTIVES,124(7),1050-1061.
MLA Leung, Maxwell C. K.,et al."Systems Toxicology of Male Reproductive Development: Profiling 774 Chemicals for Molecular Targets and Adverse Outcomes".ENVIRONMENTAL HEALTH PERSPECTIVES 124.7(2016):1050-1061.
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