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饮食中给予小鼠柠檬黄的生殖和神经行为毒性研究。

Reproductive and neurobehavioural toxicity study of tartrazine administered to mice in the diet.

作者信息

Tanaka Toyohito

机构信息

Department of Environmental Health and Toxicology, Tokyo Metropolitan Institute of Public Health, 3-24-1, Hyakunincho, Shinjuku-ku, Tokyo 169-0073, Japan.

出版信息

Food Chem Toxicol. 2006 Feb;44(2):179-87. doi: 10.1016/j.fct.2005.06.011. Epub 2005 Aug 8.

Abstract

Tartrazine was given in the diet to provide levels of 0% (control), 0.05%, 0.15%, and 0.45% (approximately 83, 259, 773 mg/kg/day, respectively) from five weeks of age of the F0 generation to nine weeks of age of the F1 generation in mice, and selected reproductive and neurobehavioural parameters were measured. In movement activity of exploratory behaviour in the F0 generation, number of vertical activity was significantly increased in the middle-dose group in males. There were no adverse effects of tartrazine on either litter size, litter weight and sex ratio at birth. The average body weight of male offspring was significantly increased in the high-dose group and that of female offspring was significantly increased in the middle-dose group at birth. In behavioural developmental parameters, surface righting at PND 4 was significantly accelerated in the high-dose group in male offspring, and those effects were significantly dose-related in a trend test (P<0.01). Cliff avoidance at PND 7 was significantly accelerated in the middle-dose group in male offspring. Negative geotaxis at PND 4 was significantly delayed in the high-dose group in female offspring. Other variables measured showed no significant adverse effects in either sex in the lactation period. In movement activity of exploratory behaviour in the F1 generation, number of movement showed a significant tendency to be affected in the treatment groups in male offspring in a trend test (P<0.05). The dose level of tartrazine in the present study produced a few adverse effects in neurobehavioural parameters during the lactation period in mice. Nevertheless, the high-dose level were in excess of the ADI of tartrazine (0-7.5 mg/kgbw), and the actual dietary intake of tartrazine is presumed to be much lower. It would therefore appear that the levels of actual dietary intake of tartrazine is unlikely to produce any adverse effects in humans.

摘要

在小鼠中,从F0代5周龄到F1代9周龄,在饮食中添加柠檬黄,使其含量分别为0%(对照)、0.05%、0.15%和0.45%(分别约为83、259、773毫克/千克/天),并测量选定的生殖和神经行为参数。在F0代探索行为的运动活动中,雄性中剂量组的垂直活动次数显著增加。柠檬黄对产仔数、出生时的窝重和性别比例均无不良影响。出生时,高剂量组雄性后代的平均体重显著增加,中剂量组雌性后代的平均体重显著增加。在行为发育参数方面,雄性后代高剂量组在出生后第4天的表面翻正显著加速,在趋势检验中这些影响与剂量显著相关(P<0.01)。雄性后代中剂量组在出生后第7天的悬崖回避显著加速。雌性后代高剂量组在出生后第4天的负趋地性显著延迟。所测量的其他变量在哺乳期对两性均未显示出显著的不良影响。在F1代探索行为的运动活动中,在趋势检验中,雄性后代治疗组的运动次数有显著受影响的趋势(P<0.05)。本研究中柠檬黄的剂量水平在小鼠哺乳期对神经行为参数产生了一些不良影响。然而,高剂量水平超过了柠檬黄的每日允许摄入量(0-7.5毫克/千克体重),并且推测柠檬黄的实际饮食摄入量要低得多。因此,似乎柠檬黄的实际饮食摄入量水平不太可能对人类产生任何不良影响。

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