GENE EXPRESSION PROFILING OF RAT LIVER TREATED WITH SERUM TRIGLYCERIDE-DECREASING COMPOUNDS
スポンサーリンク
概要
- 論文の詳細を見る
We have constructed a large-scale transcriptome database of rat liver treated with various drugs. In an effort to identify a biomarker for interpretation of plasma triglyceride (TG) decrease, we extracted 218 probe sets of rat hepatic genes from data of 15 drugs that decreased the plasma TG level but differentially affected food consumption. Pathway and gene ontology analysis revealed that the genes belong to amino acid metabolism, lipid metabolism and xenobiotics metabolism. Principal component analysis (PCA) showed that 12 out of 15 compounds were separated in the direction of PC1, and these 12 were separated in the direction of PC2, according to their hepatic gene expression profiles. It was found that genes with either large or small eigenvector values in principal component PC 2 were those reported to be regulated by peroxisome proliferator-activated receptor (PPAR)α or constitutive androstane receptor (CAR), respectively. In fact, WY-14,643, clofibrate, gemfibrozil and benzbromarone, reported to be PPARα activators, distributed to the former, whereas propylthiouracil, omeprazole, phenobarbital, thioacetamide, methapyrilene, sulfasalazine and coumarin did to the latter. We conclude that these identified 218 probe sets could be a useful source of biomarkers for classification of plasma TG decrease, based on the mechanisms involving PPARα and CAR.
- 日本トキシコロジー学会の論文
- 2007-10-15
著者
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NAGAO Taku
National Institute of Health Sciences
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Nagao Taku
Food Safety Commission Of Japan
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Nagao Taku
Laboratory Of Pharmacology & Toxicology Graduate School Of Pharmaceutical Sciences The Universit
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Nagao Taku
Laboratory Of Pharmacology And Toxicology Graduate School Of Pharmaceutical Sciences The University
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Ono Atsushi
Toxicogenomics Project National Institute Of Biomedical Innovation:national Institute Of Health Scie
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Kiyosawa Naoki
Toxicogenomics Project National Inst. Of Biomedical Innovation
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Kiyosawa Naoki
Toxicogenomics Project National Institute Of Biomedical Innovation
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Miwa Satoko
Exploratory Toxicology & Dmpk Research Laboratories Tanabe Seiyaku Co. Ltd.
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MIYAGISHIMA Toshikazu
Toxicogenomics Project, National Institute of Biomedical Innovation
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URUSHIDANI Tetsuro
Toxicogenomics Project, National Institute of Biomedical Innovation
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Shimizu Toshinobu
Toxicology Laboratory, Pharmaceuticals Research Unit, Research & Development Division, Mitsubishi Ph
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Suzuki Takamasa
Toxicogenomics Project National Institute Of Biomedical Innovation
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Urushidani Tetsuro
Toxicogenomics Project National Institute Of Biomedical Innovation:department Of Pathophysiology Dos
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Urushidani Tetsuro
Laboratory Of Pharmacology & Toxicology Graduate School Of Pharmaceutical Sciences The Universit
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Miyagishima Toshikazu
Toxicogenomics Project National Institute Of Biomedical Innovation
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Uehara Takeki
Toxicogenomics Project National Institute Of Biomedical Innovation
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OMURA Ko
Toxicogenomics Project, National Institute of Biomedical Innovation
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HIRODE Mitsuhiro
Toxicogenomics Project, National Institute of Biomedical Innovation
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Omura Ko
Toxicogenomics Project National Institute Of Biomedical Innovation
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Shimizu Toshinobu
Toxicogenomics Project National Institute Of Biomedical Innovation
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Nagao Taku
National Institute Of Health Sci.
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Hirode Mitsuhiro
Toxicogenomics Project National Institute Of Biomedical Innovation
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Ono Atsushi
Toxicogenomics Project National Institute Of Biomedical Innovation:national Institute Of Health Scie
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Urushidani Tetsuro
Toxicogenomics Project National Institute Of Biomedical Innovation
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