Identification of an adverse outcome pathway (AOP) for chemical-induced craniofacial anomalies using the transgenic zebrafish model

Author:

Liu Shujie1,Kawanishi Toru23ORCID,Shimada Atsuko2,Ikeda Naohiro4,Yamane Masayuki1,Takeda Hiroyuki25ORCID,Tasaki Junichi4ORCID

Affiliation:

1. R&D, Safety Science Research, Kao Corporation , Tochigi 321-3497, Japan

2. Department of Biological Sciences, Graduate School of Science, University of Tokyo , Tokyo 113-0033, Japan

3. School of Life Science and Technology, Tokyo Institute of Technology , Kanagawa 226-8501, Japan

4. R&D, Safety Science Research, Kao Corporation , Kanagawa 210-0821, Japan

5. Faculty of Life Sciences, Kyoto Sangyo University , Kyoto 603-8555, Japan

Abstract

Abstract Craniofacial anomalies are one of the most frequent birth defects worldwide and are often caused by genetic and environmental factors such as pharmaceuticals and chemical agents. Although identifying adverse outcome pathways (AOPs) is a central issue for evaluating the teratogenicity, the AOP causing craniofacial anomalies has not been identified. Recently, zebrafish has gained interest as an emerging model for predicting teratogenicity because of high throughput, cost-effectiveness and availability of various tools for examining teratogenic mechanisms. Here, we established zebrafish sox10-EGFP reporter lines to visualize cranial neural crest cells (CNCCs) and have identified the AOPs for craniofacial anomalies. When we exposed the transgenic embryos to teratogens that were reported to cause craniofacial anomalies in mammals, CNCC migration and subsequent morphogenesis of the first pharyngeal arch were impaired at 24 hours post-fertilization. We also found that cell proliferation and apoptosis of the migratory CNCCs were disturbed, which would be key events of the AOP. From these results, we propose that our sox10-EGFP reporter lines serve as a valuable model for detecting craniofacial skeletal abnormalities, from early to late developmental stages. Given that the developmental process of CNCCs around this stage is highly conserved between zebrafish and mammals, our findings can be extrapolated to mammalian craniofacial development and thus help in predicting craniofacial anomalies in human.

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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