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用风化原油和一种分散剂对费希尔344大鼠进行口服治疗会影响肠道代谢和微生物群。

Oral treatment of Fischer 344 rats with weathered crude oil and a dispersant influences intestinal metabolism and microbiota.

作者信息

George S E, Nelson G M, Kohan M J, Warren S H, Eischen B T, Brooks L R

机构信息

Environmental Carcinogenesis Division, US Environmental Protection Agency, Research Triangle Park, North Carolina 27711, USA. george.elizabeth@ epa.gov

出版信息

J Toxicol Environ Health A. 2001 Jun 22;63(4):297-316. doi: 10.1080/15287390151143686.

Abstract

When oil is spilled into aquatic systems, chemical dispersants frequently are applied to enhance emulsification and biological availability. In this study, a mammalian model system was used to determine the effect of Bonnie Light Nigerian crude oil, weathered for 2 d with continuous spraying and recirculation, and a widely used dispersant, Corexit (Cx) 9527, on intestinal microbial metabolism and associated populations. To determine the subchronic dose, concentrated or diluted (1:2, 1:5, 1:10, 1:20) Cx9527 or oil was administered by gavage to Fischer 344 rats and the effect on body weight was determined. Next, rats were treated for 5 wk with oil, dispersant, or dispersant + oil. Body and tissue weights, urine mutagenicity, and the impact on the intestinal microflora and three microbial intestinal enzymes linked to bioactivation were determined in the small and large intestines and cecum. Two tested dispersants, Cx9527 and Cx9500, were toxic in vitro (1:1,000 dilution), and oil was not mutagenic in strains TA98 and TA100(+/-S9). None of the treated rats produced urine mutagens detected by TA98 or TA100. Undiluted dispersant was lethal to rats, and weight changes were observed depending on the dilution, whereas oil generally was not toxic. In the 5-wk study, body and tissue weights were unaffected at the doses administered. Small-intestinal levels of azoreductase (AR), beta-glucuronidase (BG), and nitroreductase (NR) were considerably lower than cecal and large-intestinal activities at the same time point. A temporal increase in AR activity was observed in control animals in the 3 tissues examined, and large-intestinal BG activity was elevated in 3-wk controls. No significant changes in cecal BG activity were observed. Oil- or dispersant-treated rats had mixed results with reduced activity at 3 wk and elevated activity at 5 wk compared to controls. However, when the dispersant was combined with oil at 3 wk, a reduction in activity was observed that was similar to that of dispersant alone. One-week nitroreductase activity in the small intestine and cecum was unaffected in the three treatment groups, but elevated activity was observed in the large intestines of animals treated with oil or dispersant. The effect of the combination dose was not significantly different from the control value. Due to experimental error, no 3- or 5-wk NR data were available. By 5 wk of treatment, enterobacteria and enterococci were eliminated from ceca of oil-treated rats. When oil was administered in combination with dispersant, an apparent protective effect was observed on the enterococci and lactose-fermenting and nonfermenting enterobacteria. A more detailed analysis at the species level revealed qualitative differences dependent on the treatment. This study suggests that prolonged exposure of mammals to oil, dispersant, or in combination impacts intestinal metabolism, which ultimately could lead to altered detoxification of oil constituents and coexposed toxicants.

摘要

当石油泄漏到水生系统中时,通常会使用化学分散剂来增强乳化作用和生物可利用性。在本研究中,使用了一个哺乳动物模型系统来确定经过连续喷洒和再循环风化2天的邦妮轻质尼日利亚原油以及一种广泛使用的分散剂科雷希特(Cx)9527对肠道微生物代谢及相关菌群的影响。为了确定亚慢性剂量,将浓缩或稀释(1:2、1:5、1:10、1:20)的Cx9527或油经口灌胃给予Fischer 344大鼠,并测定其对体重的影响。接下来,用石油、分散剂或分散剂+石油对大鼠进行5周的处理。测定了大鼠的体重和组织重量、尿液致突变性以及对小肠、大肠和盲肠中肠道微生物群和三种与生物活化相关的微生物肠道酶的影响。两种测试的分散剂Cx9527和Cx9500在体外(1:1000稀释)具有毒性,而石油在TA98和TA100菌株(±S9)中无致突变性。经处理的大鼠均未产生TA98或TA100检测到的尿液致突变物。未稀释的分散剂对大鼠具有致死性,根据稀释度观察到体重变化,而石油一般无毒。在为期5周的研究中,所给予剂量对体重和组织重量没有影响。在同一时间点,小肠中的偶氮还原酶(AR)、β-葡萄糖醛酸酶(BG)和硝基还原酶(NR)水平明显低于盲肠和大肠中的活性。在检查的3个组织中,对照动物的AR活性随时间增加,3周龄对照组的大肠BG活性升高。未观察到盲肠BG活性有显著变化。与对照组相比,经石油或分散剂处理的大鼠结果不一,3周时活性降低,5周时活性升高。然而,当分散剂与石油在3周时联合使用时,观察到活性降低,与单独使用分散剂时相似。三个处理组中小肠和盲肠的一周硝基还原酶活性未受影响,但在用石油或分散剂处理的动物大肠中观察到活性升高。联合剂量的影响与对照值无显著差异。由于实验误差,没有3周或5周的NR数据。到处理5周时,经石油处理的大鼠盲肠中的肠杆菌和肠球菌被清除。当石油与分散剂联合使用时,对肠球菌以及乳糖发酵和非发酵肠杆菌观察到明显的保护作用。在物种水平上更详细的分析揭示了取决于处理方式的定性差异。本研究表明,哺乳动物长期暴露于石油、分散剂或两者组合会影响肠道代谢,这最终可能导致石油成分和同时暴露的毒物的解毒改变。

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