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通过饮水接触丙烯酰胺对大鼠前脑运动和感觉区域的mRNA表达及组织学完整性影响极小。

The mRNA expression and histological integrity in rat forebrain motor and sensory regions are minimally affected by acrylamide exposure through drinking water.

作者信息

Bowyer John F, Latendresse John R, Delongchamp Robert R, Warbritton Alan R, Thomas Monzy, Divine Becky, Doerge Daniel R

机构信息

US Food and Drug Administration, National Center for Toxicological Research, Division of Neurotoxicology, 3900 NCTR Road, Jefferson, AR 72079, USA.

出版信息

Toxicol Appl Pharmacol. 2009 Nov 1;240(3):401-11. doi: 10.1016/j.taap.2009.07.036. Epub 2009 Aug 5.

Abstract

A study was undertaken to determine whether alterations in the gene expression or overt histological signs of neurotoxicity in selected regions of the forebrain might occur from acrylamide exposure via drinking water. Gene expression at the mRNA level was evaluated by cDNA array and/or RT-PCR analysis in the striatum, substantia nigra and parietal cortex of rat after a 2-week acrylamide exposure. The highest dose tested (maximally tolerated) of approximately 44 mg/kg/day resulted in a significant decreased body weight, sluggishness, and locomotor activity reduction. These physiological effects were not accompanied by prominent changes in gene expression in the forebrain. All the expression changes seen in the 1200 genes that were evaluated in the three brain regions were < or =1.5-fold, and most not significant. Very few, if any, statistically significant changes were seen in mRNA levels of the more than 50 genes directly related to the cholinergic, noradrenergic, GABAergic or glutamatergic neurotransmitter systems in the striatum, substantia nigra or parietal cortex. All the expression changes observed in genes related to dopaminergic function were less than 1.5-fold and not statistically significant and the 5HT1b receptor was the only serotonin-related gene affected. Therefore, gene expression changes were few and modest in basal ganglia and sensory cortex at a time when the behavioral manifestations of acrylamide toxicity had become prominent. No histological evidence of axonal, dendritic or neuronal cell body damage was found in the forebrain due to the acrylamide exposure. As well, microglial activation was not present. These findings are consistent with the absence of expression changes in genes related to changes in neuroinflammation or neurotoxicity. Over all, these data suggest that oral ingestion of acrylamide in drinking water or food, even at maximally tolerable levels, induced neither marked changes in gene expression nor neurotoxicity in the motor and somatosensory areas of the central nervous system.

摘要

开展了一项研究,以确定通过饮用水接触丙烯酰胺是否会导致前脑特定区域的基因表达改变或明显的神经毒性组织学迹象。在大鼠经2周丙烯酰胺暴露后,通过cDNA阵列和/或RT-PCR分析评估纹状体、黑质和顶叶皮质中mRNA水平的基因表达。所测试的最高剂量(最大耐受剂量)约为44mg/kg/天,导致体重显著下降、行动迟缓以及运动活性降低。这些生理效应并未伴随前脑基因表达的显著变化。在三个脑区评估的1200个基因中观察到的所有表达变化均≤1.5倍,且大多数无统计学意义。在纹状体、黑质或顶叶皮质中,与胆碱能、去甲肾上腺素能、GABA能或谷氨酸能神经递质系统直接相关的50多个基因的mRNA水平,几乎未观察到具有统计学意义的变化。在与多巴胺能功能相关的基因中观察到的所有表达变化均小于1.5倍,且无统计学意义,5HT1b受体是唯一受影响的与血清素相关的基因。因此,在丙烯酰胺毒性的行为表现变得明显时,基底神经节和感觉皮质中的基因表达变化很少且不明显。未发现前脑因丙烯酰胺暴露而出现轴突、树突或神经元细胞体损伤的组织学证据。同样,也不存在小胶质细胞激活。这些发现与神经炎症或神经毒性变化相关基因的表达变化缺失一致。总体而言,这些数据表明,即使在最大耐受水平下,通过饮用水或食物口服摄入丙烯酰胺,也不会在中枢神经系统的运动和躯体感觉区域引起明显的基因表达变化或神经毒性。

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