p53 Contributes to Differentiating Gene Expression Following Exposure to Acetaminophen and Its Less Hepatotoxic Regioisomer Both In Vitro and In Vivo.

Gene regulation and systems biology Pub Date : 2015-06-01 eCollection Date: 2015-01-01 DOI:10.4137/GRSB.S25388
Brendan D Stamper, Michael L Garcia, Duy Q Nguyen, Richard P Beyer, Theo K Bammler, Frederico M Farin, Terrance J Kavanagh, Sidney D Nelson
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引用次数: 9

Abstract

The goal of the present study was to compare hepatic toxicogenomic signatures across in vitro and in vivo mouse models following exposure to acetaminophen (APAP) or its relatively nontoxic regioisomer 3'-hydroxyacetanilide (AMAP). Two different Affymetrix microarray platforms and one Agilent Oligonucleotide microarray were utilized. APAP and AMAP treatments resulted in significant and large changes in gene expression that were quite disparate, and likely related to their different toxicologic profiles. Ten transcripts, all of which have been implicated in p53 signaling, were identified as differentially regulated at all time-points following APAP and AMAP treatments across multiple microarray platforms. Protein-level quantification of p53 activity aligned with results from the transcriptomic analysis, thus supporting the implicated mechanism of APAP-induced toxicity. Therefore, the results of this study provide good evidence that APAP-induced p53 phosphorylation and an altered p53-driven transcriptional response are fundamental steps in APAP-induced toxicity.

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p53对暴露于对乙酰氨基酚及其肝毒性较低的区域异构体后基因表达的差异有贡献。
本研究的目的是比较体外和体内小鼠模型暴露于对乙酰氨基酚(APAP)或其相对无毒的区域异构体3'-羟基乙酰苯胺(AMAP)后的肝脏毒性基因组特征。使用了两种不同的Affymetrix微阵列平台和一种Agilent寡核苷酸微阵列。APAP和AMAP处理导致基因表达的显著和巨大变化,这些变化完全不同,可能与它们不同的毒理学特征有关。在多个微阵列平台上进行APAP和AMAP治疗后,在所有时间点发现了10个转录本,它们都与p53信号传导有关。p53活性的蛋白水平定量与转录组学分析结果一致,从而支持apap诱导毒性的相关机制。因此,本研究的结果提供了很好的证据,证明apap诱导的p53磷酸化和p53驱动的转录反应的改变是apap诱导的毒性的基本步骤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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