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饮用含低剂量丙烯酰胺的水长期处理的雄性和雌性新生大鼠的转录组学分析及激素变化

Transcriptomics analysis and hormonal changes of male and female neonatal rats treated chronically with a low dose of acrylamide in their drinking water.

作者信息

Collí-Dulá Reyna Cristina, Friedman Marvin A, Hansen Benjamin, Denslow Nancy D

机构信息

Department of Physiological Sciences and Center for Environmental and Human Toxicology, University of Florida, Gainesville, FL 32611, USA.

Kennesaw State University, Kennesaw, GA 30144, USA.

出版信息

Toxicol Rep. 2016 Mar 19;3:414-426. doi: 10.1016/j.toxrep.2016.03.009. eCollection 2016.

Abstract

Acrylamide is known to produce follicular cell tumors of the thyroid in rats. RccHan Wistar rats were exposed to a carcinogenic dose of acrylamide (3 mg/Kg bw/day) from gestation day 6 to delivery and then through their drinking water to postnatal day 35. In order to identify potential mechanisms of carcinogenesis in the thyroid glands, we used a transcriptomics approach. Thyroid glands were collected from male pups at 10 PM and female pups at 10 AM or 10 PM in order to establish whether active exposure to acrylamide influenced gene expression patterns or pathways that could be related to carcinogenesis. While all animals exposed to acrylamide showed changes in expected target pathways related to carcinogenesis such as DNA repair, DNA replication, chromosome segregation, among others; animals that were sacrificed while actively drinking acrylamide-laced water during their active period at night showed increased changes in pathways related to oxidative stress, detoxification pathways, metabolism, and activation of checkpoint pathways, among others. In addition, thyroid hormones, triiodothyronine (T3) and thyroxine (T4), were increased in acrylamide-treated rats sampled at night, but not in quiescent animals when compared to controls. The data clearly indicate that time of day for sample collection is critical to identifying molecular pathways that are altered by the exposures. These results suggest that carcinogenesis in the thyroids of acrylamide treated rats may ensue from several different mechanisms such as hormonal changes and oxidative stress and not only from direct genotoxicity, as has been assumed to date.

摘要

已知丙烯酰胺可在大鼠中诱发甲状腺滤泡细胞肿瘤。将RccHan Wistar大鼠从妊娠第6天至分娩期间暴露于致癌剂量的丙烯酰胺(3毫克/千克体重/天),然后通过饮用水持续暴露至出生后第35天。为了确定甲状腺致癌的潜在机制,我们采用了转录组学方法。在晚上10点采集雄性幼崽的甲状腺,在上午10点或晚上10点采集雌性幼崽的甲状腺,以确定丙烯酰胺的主动暴露是否会影响与致癌作用相关的基因表达模式或信号通路。虽然所有暴露于丙烯酰胺的动物在与致癌作用相关的预期目标信号通路中都出现了变化,如DNA修复、DNA复制、染色体分离等;但在夜间活跃期主动饮用含丙烯酰胺水时被处死的动物,在与氧化应激、解毒途径、代谢以及检查点信号通路激活等相关的信号通路中出现了更多变化。此外,在夜间采集的丙烯酰胺处理大鼠中,甲状腺激素三碘甲状腺原氨酸(T3)和甲状腺素(T4)有所增加,但与对照组相比,在静止期动物中未出现这种情况。数据清楚地表明,样本采集的时间对于识别因暴露而改变的分子信号通路至关重要。这些结果表明,丙烯酰胺处理大鼠甲状腺的致癌作用可能源于多种不同机制,如激素变化和氧化应激,而不仅仅是迄今为止所认为的直接基因毒性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/07f7/5615912/a081a8cb2095/gr1.jpg

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