New Short Term Prediction Method for Chemical Carcinogenicity by Hepatic Transcript Profiling following 28-Day Toxicity Tests in Rats

Author:

Matsumoto Hiroshi1,Yakabe Yoshikuni1,Saito Fumiyo1,Saito Koichi2,Sumida Kayo2,Sekijima Masaru3,Nakayama Koji3,Miyaura Hideki1,Otsuka Masanori1,Shirai Tomoyuki4

Affiliation:

1. Chemicals Assessment and Research Center, Chemicals Evaluation and Research Institute, Japan, 1600 Shimotakano, Sugito-machi, Kitakatsushika-gun, Saitama 345–0043, Japan.

2. Sumitomo Chemical Co., Ltd., 1-98, 3-Chome, Kasugade-Naka, Konohana-ku, Osaka 554–8558, Japan.

3. Advanced Medical Science Research Center, Mitsubishi Chemical Medience Corporation, 14 Sunayama, Kamisu, Ibaragi, Japan.

4. Department of Experimental Pathology and Tumor Biology, Nagoya City University graduate School of Medical Sciences, 1 Kawasumi, Mizuho-cho, Nagoya, 467–8601, Japan.

Abstract

We have previously shown the hepatic gene expression profiles of carcinogens in 28-day toxicity tests were clustered into three major groups (Group-1 to 3). Here, we developed a new prediction method for Group-1 carcinogens which consist mainly of genotoxic rat hepatocarcinogens. The prediction formula was generated by a support vector machine using 5 selected genes as the predictive genes and predictive score was introduced to judge carcinogenicity. It correctly predicted the carcinogenicity of all 17 Group-1 chemicals and 22 of 24 non-carcinogens regardless of genotoxicity. In the dose-response study, the prediction score was altered from negative to positive as the dose increased, indicating that the characteristic gene expression profile emerged over a range of carcinogen-specific doses. We conclude that the prediction formula can quantitatively predict the carcinogenicity of Group-1 carcinogens. The same method may be applied to other groups of carcinogens to build a total system for prediction of carcinogenicity.

Publisher

SAGE Publications

Subject

Cancer Research,Oncology

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