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(사)한국바이오칩학회 The Korean BioChip Society



BT+IT+NTThe Korean BioChip Society

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Info. Vol.3 - No.1 (2009.03.20)
Title Analysis of Gene Expression in the Testes of Mice Exposed to Bisphenol A and Nonylphenol
Authors Jung-Hwa Oh1, Moon-Ju Oh2, Han-Jin Park1, Seung Jun Kim2, Se-Myo Park1, Hea-Jin Yoon1, Jae-Woo Cho3, Seung Yong Hwang2 & Seokjoo Yoon1
Institutions 1Toxicogenomics Team, 3Clinical Pathology Team, Korea Institute of Toxicology, 19 Shinsung-ro, Yuseong, Daejeon 305-343, Korea
2GenoCheck Co., Ltd. & Hanyang University, Sa 3-dong, Sangnok-gu, Ansan, Gyeonggi-do 426-791, Korea
Correspondence and requests for materials should be addressed to S. Yoon (sjyoon@kitox.re.kr)
Abstract Estrogenic environmental compounds (xenoestrogens) have adverse effects on male reproductive systems, including decreased sperm counts and problems with reproductive development. Although the male reproductive toxicity induced by xenoestrogens has been investigated, the molecular mechanisms by which estrogenic compounds induce toxicity in testes are unclear. This study used a microarray analysis to examine testicular toxicity and gene expression profiles in mice after 30 days of exposure to two estrogenic compounds, bisphenol A (BPA) and nonylphenol (NP). In total, 275 and 729 genes were identified as being either up- or down-regulated, with over 1.5-fold changes, in the testes of the BPAand NP-treated groups, respectively. Differentially expressed genes were classified using a k-means clustering algorithm, and their biological functions and canonical pathways were further analyzed using Ingenuity Pathways Analysis (IPA). Toxicological function analysis characterized the mode of action according to BPA and NP. Pathway analysis identified genes involved in gluconeogenesis and calcium signaling in the BPA-treated group and genes involved in Wnt/棺-catenin and estrogen receptor signaling in the NP-treated group. In addition, several differentially expressed genes that may play a role in spermatogenesis, such as Odf1 and the Sox family, were identified. Collectively, these data help to elucidate the molecular mechanism of reproductive toxicity induced by xenoestrogens.
Keyword Xenoestrogens, Bisphenol A, Nonylphenol, Gene expression profiling, Reproductive toxicity
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