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伏马菌素B1对怀孕大鼠的影响。

Effects of fumonisin B1 in pregnant rats.

作者信息

Collins T F, Shackelford M E, Sprando R L, Black T N, Láborde J B, Hansen D K, Eppley R M, Trucksess M W, Howard P C, Bryant M A, Ruggles D I, Olejnik N, Rorie J I

机构信息

Center for Food Safety and Applied Nutrition, Food and Drug Administration, Laurel, MD 20708, USA.

出版信息

Food Chem Toxicol. 1998 May;36(5):397-408. doi: 10.1016/s0278-6915(97)00170-1.

Abstract

Fumonisin B1 (FB1), the major mycotoxin from Fusarium moniliforme, has been implicated as a causative agent in several animal and human diseases. Despite animal toxicity studies and human epidemiological studies of FB1, knowledge of its reproductive effects is scarce. In this study, one of a series of proposed studies that will allow extrapolation to humans, pregnant rats were given oral doses of 0, 1.875, 3.75, 7.5 or 15 mg FB1/kg on gestation days 3 16. Caesarean sections were performed on day 17 or 20, and maternal condition, implantation efficiency, foetal viability and foetal development were measured. Dose-related decreases in overall feed consumption and body weight gain were seen, but only the feed consumption decrease at 15 mg/kg, and the decreased body weight gain at 15 mg/kg on days 0-17 were statistically significant. Foetal body weights at day 17 were similar in control and treated groups; but in day-20 foetuses, female weight and crown-rump length were significantly decreased at 15 mg/kg. FB1 was not teratogenic at the doses tested, and no dose-related effects were seen in either skeletal or soft-tissue development. In day-17 animals, maternal and foetal brain, liver and kidney tissues, and maternal serum were preserved to study the levels of sphinganine (Sa), sphingosine (So), and the Sa/So ratios. Dose-related increases were seen in Sa/So ratios in maternal livers, kidneys and serum. Sa/So ratios of maternal brains were not affected, nor were those of foetal kidneys, livers or brains.

摘要

伏马菌素B1(FB1)是串珠镰刀菌产生的主要霉菌毒素,被认为是多种动物和人类疾病的致病因子。尽管已经对FB1进行了动物毒性研究和人类流行病学研究,但其对生殖系统的影响仍知之甚少。在本研究中,作为一系列旨在推断对人类影响的拟议研究之一,在妊娠第3至16天给怀孕大鼠口服0、1.875、3.75、7.5或15 mg FB1/kg的剂量。在第17天或第20天进行剖腹产,并测量母体状况、着床效率、胎儿活力和胎儿发育情况。观察到总体饲料消耗量和体重增加呈剂量相关下降,但仅15 mg/kg剂量下饲料消耗量的下降以及第0至17天15 mg/kg剂量下体重增加的下降具有统计学意义。第17天对照组和处理组的胎儿体重相似;但在第20天的胎儿中,15 mg/kg剂量下雌性胎儿体重和顶臀长度显著下降。在所测试的剂量下,FB1没有致畸性,在骨骼或软组织发育方面也未观察到剂量相关影响。在第17天的动物中,保存母体和胎儿的脑、肝和肾组织以及母体血清,以研究鞘氨醇(Sa)、鞘氨醇(So)的水平以及Sa/So比值。在母体肝脏、肾脏和血清中观察到Sa/So比值呈剂量相关增加。母体脑的Sa/So比值未受影响,胎儿肾脏、肝脏或脑的比值也未受影响。

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