利用毒物基因组学方法评估全氟辛酸诱导雄性 Sprague-Dawley 大鼠肝脏肿瘤的作用模式。

IF 1.2 4区 环境科学与生态学 Q4 ENVIRONMENTAL SCIENCES
Xilin Li, Zemin Wang, Qiangen Wu, James E Klaunig
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引用次数: 0

摘要

全氟辛酸(PFOA)诱发大鼠肝脏肿瘤的作用模式(MOA)被认为涉及过氧化物酶体增殖激活受体α(PPARα)的激动作用。尽管在啮齿类动物肝脏中有明确的 PPARα 激活证据,但细胞生长的驱动机制仍然难以捉摸。在此,我们使用剂量反应性顶端终点和转录组数据来研究拟议的作用方式。雄性 Sprague-Dawley 大鼠通过口服方式分别接受 0、1、5 和 15 mg/kg PFOA 治疗 7、14 和 28 天。结果表明,PFOA 可诱导大鼠肝脏肿大和肝细胞肥大。PPARα 以剂量依赖的方式被激活。毒物基因组分析显示,PPARα激活后会出现六种早期生物标志物(Cyp4a1、Nr1d1、Acot1、Acot2、Ehhadh和Vnn1)。肝细胞 DNA 合成出现短暂上升,而 Ki-67 标记指数没有变化。转录组分析表明,与 DNA 合成、细胞凋亡或细胞周期相关的通路没有明显的富集。包括 Ccnd1、Ccnb1、Ccna2 和 Ccne2 在内的关键细胞周期蛋白受到 PFOA 的剂量依赖性抑制。氧化应激和核因子-κB 信号通路未受影响。总之,在研究的时间范围内,PFOA 诱导肝细胞增殖的证据是短暂的。我们的研究结果强调,在评估全氟辛酸对人类的致癌风险时,必须考虑物种间的差异和特定化学品的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Evaluating the mode of action of perfluorooctanoic acid-induced liver tumors in male Sprague-Dawley rats using a toxicogenomic approach.

The mode of action (MOA) underlying perfluorooctanoic acid (PFOA)-induced liver tumors in rats is proposed to involve peroxisome proliferator-activated receptor α (PPARα) agonism. Despite clear PPARα activation evidence in rodent livers, the mechanisms driving cell growth remain elusive. Herein, we used dose-responsive apical endpoints and transcriptomic data to examine the proposed MOA. Male Sprague-Dawley rats were treated with 0, 1, 5, and 15 mg/kg PFOA for 7, 14, and 28 days via oral gavage. We showed PFOA induced hepatomegaly along with hepatocellular hypertrophy in rats. PPARα was activated in a dose-dependent manner. Toxicogenomic analysis revealed six early biomarkers (Cyp4a1, Nr1d1, Acot1, Acot2, Ehhadh, and Vnn1) in response to PPARα activation. A transient rise in hepatocellular DNA synthesis was demonstrated while Ki-67 labeling index showed no change. Transcriptomic analysis indicated no significant enrichment in pathways related to DNA synthesis, apoptosis, or the cell cycle. Key cyclins including Ccnd1, Ccnb1, Ccna2, and Ccne2 were dose-dependently suppressed by PFOA. Oxidative stress and the nuclear factor-κB signaling pathway were unaffected. Overall, evidence for PFOA-induced hepatocellular proliferation was transient within the studied timeframe. Our findings underscore the importance of considering inter-species differences and chemical-specific effects when evaluating the carcinogenic risk of PFOA in humans.

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CiteScore
4.60
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