Literature DB >> 17202762

Gene expression profile in liver of differing ages of rats after single oral administration of acetaminophen.

Katsumi Morishita1, Yumiko Mizukawa, Toshihiko Kasahara, Manabu Okuyama, Kayoko Takashima, Naoki Toritsuka, Toshikazu Miyagishima, Taku Nagao, Tetsuro Urushidani.   

Abstract

In order to verify the influence of the rat age on hepatotoxicity, male Sprague-Dawley rats of 6 (young) and 12 (adult) weeks of age were orally administered acetaminophen (APAP), isoniazid (INH), or carbon tetrachloride (CCl4). Liver samples were obtained in a time-course manner, and changes in gene expression examined by an Affymetrix GeneChip. APAP caused more prominent hepatic injury with respect to pathology and blood biochemistry in adults than in young rats, whereas no obvious age-related differences were observed in INH- or CCl4-treated rats. Comparing gene expression in control rats, CYP3A13 was higher and GSTY2c was lower in adults, suggesting that production of the active metabolite of APAP is higher and its detoxification is lower in adults. The total amount of glutathione and total SH in rat liver was found to be higher in adult rats whereas the extent of its reduction by APAP was larger in adults. A detailed analysis of genes showing age-related differences revealed that some of them were different not in their extent but in their time course, i.e., the stress responses occurred earlier in the young than in the adult, resulting in a difference at 24 hr after dosing. These results suggest that the age-related difference in toxicity would be attributed to a higher expression of CYP3A13, producing the active metabolite of APAP as well as the lower expression of the detoxification enzyme, GSTY2c, in adult rats. Furthermore, these differences affect the time course of APAP toxicity. The present study clearly depicts the advantage of the multi-time, multi-dose protocol employed in our project for analyzing the mechanism of toxicity by gene expression profiling.

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Year:  2006        PMID: 17202762     DOI: 10.2131/jts.31.491

Source DB:  PubMed          Journal:  J Toxicol Sci        ISSN: 0388-1350            Impact factor:   2.196


  6 in total

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Journal:  Toxicol Appl Pharmacol       Date:  2019-04-08       Impact factor: 4.219

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3.  Multiple microRNAs function as self-protective modules in acetaminophen-induced hepatotoxicity in humans.

Authors:  Dianke Yu; Leihong Wu; Pritmohinder Gill; William H Tolleson; Si Chen; Jinchun Sun; Bridgett Knox; Yaqiong Jin; Wenming Xiao; Huixiao Hong; Yong Wang; Zhen Ren; Lei Guo; Nan Mei; Yongli Guo; Xi Yang; Leming Shi; Yinting Chen; Linjuan Zeng; Kostiantyn Dreval; Volodymyr Tryndyak; Igor Pogribny; Hong Fang; Tieliu Shi; Sandra McCullough; Sudeepa Bhattacharyya; Laura Schnackenberg; William Mattes; Richard D Beger; Laura James; Weida Tong; Baitang Ning
Journal:  Arch Toxicol       Date:  2017-10-24       Impact factor: 5.153

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Journal:  Environ Health Toxicol       Date:  2012-04-26

5.  Toxicogenomic biomarkers for liver toxicity.

Authors:  Naoki Kiyosawa; Yosuke Ando; Sunao Manabe; Takashi Yamoto
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6.  The effect of extra virgin olive oil and soybean on DNA, cytogenicity and some antioxidant enzymes in rats.

Authors:  Thanaa A El-Kholy; Mohammad Abu Hilal; Hatim Ali Al-Abbadi; Abdulhalim Salim Serafi; Ahmad K Al-Ghamdi; Hanan M Sobhy; John R C Richardson
Journal:  Nutrients       Date:  2014-06-23       Impact factor: 5.717

  6 in total

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