Integrating Publicly Available Data to Generate Computationally Predicted Adverse Outcome Pathways for Fatty Liver

被引:57
作者
Bell, Shannon M. [1 ,2 ,3 ]
Angrish, Michelle M. [2 ]
Wood, Charles E. [2 ]
Edwards, Stephen W. [2 ]
机构
[1] Oak Ridge Inst Sci & Educ, Oak Ridge, TN USA
[2] US EPA, Integrated Syst Toxicol Div, Natl Hlth & Environm Effects Res Lab, Off Res & Dev, Res Triangle Pk, NC 27711 USA
[3] NTP Interagcy Ctr Evaluat Alternat Toxicol Method, Res Triangle Pk, NC USA
关键词
computationally predicted adverse outcome pathways; cpAOP; TG-GATEs; network integration; fatty liver; steatosis; CARBON-TETRACHLORIDE; ONTOLOGY; DISEASE; IDENTIFICATION; STRATEGIES; FRAMEWORK; CHEMICALS; BIOLOGY; OBESITY;
D O I
10.1093/toxsci/kfw017
中图分类号
R99 [毒物学(毒理学)];
学科分类号
100405 [卫生毒理学];
摘要
New in vitro testing strategies make it possible to design testing batteries for large numbers of environmental chemicals. Full utilization of the results requires knowledge of the underlying biological networks and the adverse outcome pathways (AOPs) that describe the route from early molecular perturbations to an adverse outcome. Curation of a formal AOP is a time-intensive process and a rate-limiting step to designing these test batteries. Here, we describe a method for integrating publicly available data in order to generate computationally predicted AOP (cpAOP) scaffolds, which can be leveraged by domain experts to shorten the time for formal AOP development. A network-based workflow was used to facilitate the integration of multiple data types to generate cpAOPs. Edges between graph entities were identified through direct experimental or literature information, or computationally inferred using frequent itemset mining. Data from the TG-GATEs and ToxCast programs were used to channel large-scale toxicogenomics information into a cpAOP network (cpAOPnet) of over 20 000 relationships describing connections between chemical treatments, phenotypes, and perturbed pathways as measured by differential gene expression and high-throughput screening targets. The resulting fatty liver cpAOPnet is available as a resource to the community. Subnetworks of cpAOPs for a reference chemical (carbon tetrachloride, CCl4) and outcome (fatty liver) were compared with published mechanistic descriptions. In both cases, the computational approaches approximated the manually curated AOPs. The cpAOPnet can be used for accelerating expert-curated AOP development and to identify pathway targets that lack genomic markers or high-throughput screening tests. It can also facilitate identification of key events for designing test batteries and for classification and grouping of chemicals for follow up testing.
引用
收藏
页码:510 / 520
页数:11
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