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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Effect of micelle fatty acid composition and 3,4,3', 4'-tetrachlorobiphenyl (TCB) exposure on intestinal ((14)C)-TCB bioavailability and biotransformation in channel catfish in situ preparations.
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Effect of micelle fatty acid composition and 3,4,3', 4'-tetrachlorobiphenyl (TCB) exposure on intestinal ((14)C)-TCB bioavailability and biotransformation in channel catfish in situ preparations.

机译:胶束脂肪酸组成和3,4,3',4'-四氯联苯(TCB)暴露对channel鱼原位制剂中肠道((14)C)-TCB生物利用度和生物转化的影响。

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摘要

Polychlorinated biphenyls are transferred in the diet along aquatic food chains. This study investigated the effect of dietary micelle composition and 3,4,3',4'-tetrachlorobiphenyl (TCB) exposure upon the subsequent systemic bioavailability and intestinal metabolism of [(14)C]-TCB in a catfish in situ intestinal preparation. Initial in vitro experiments examined the solubility of [(14)C]-TCB in micelles of varying fatty acid composition. Micelles composed of single fatty acids demonstrated greater [(14)C]-TCB solubility with those fatty acids of longer chain length. Similarly, micelles of the long-chain fatty acid, linoleic acid, solubilized more [(14)C]-TCB than mixed micelles formulated from equal amounts of myristic (14:0), palmitic (16:0), stearic (18:0), or linoleic (18:2) acids. Systemic bioavailability of [(14)C]-TCB (60 &mgr;M) from an in situ perfused intestinal preparation was 2.2-fold greater when delivered to the intestine in linoleic acid micelles as compared to the mixed micelle preparation. Catfish exposed in vivo to either 0.5 or 5.0 mg TCB/kg feed for 10 days resulted in a 45 to 47% decrease in the subsequent systemic bioavailability of [(14)C]-TCB in the in situ intestinal preparation. Total intestinal cytochrome P450 content was not significantly affected by TCB preexposure. Immunodetectable CYP1A was found only in the 5.0 mg TCB/kg diet treatment. Corresponding intestinal aryl hydrocarbon hydroxylase (AHH) activities were 2.46 +/- 1.16, 2.43 +/- 1.58, and 11.35 +/- 10.25 pmol/min/mg protein for the control, 0.5, and 5 mg TCB/kg diet groups, respectively. [(14)C]-TCB in the in situ preparation was metabolized to only a small degree upon a single pass through the intestinal mucosa of the catfish. High variability and low rates of metabolism precluded the association of the magnitude of metabolism with dietary TCB pretreatment. Analysis of tissue sample extracts demonstrated 4 minor peaks, 3 of which were tentatively identified by co-elution with standards as 2-OH-3,4,3',4'-TCB, 4-OH-3,5,3',4'-TCB, and 5-OH-3, 4,3',4'-TCB. A fourth remains unidentified. Histological changes in the intestine such as thinning of the submucosa and increased numbers of goblet cells were evident at the 5.0 mg TCB/kg diet dose. These results suggest that TCB intestinal bioavailability may be linked to micelle composition as well as TCB exposure history. Furthermore, single pass intestinal metabolism appears to be a minor contributor to the biotransformational modification of dietary TCB.
机译:日粮中的多氯联苯沿着水生食物链转移。这项研究调查了饮食胶束组成和3,4,3',4'-四氯联苯(TCB)暴露对subsequent鱼原位肠道制剂中[(14)C] -TCB后续系统生物利用度和肠道代谢的影响。最初的体外实验检查了[(14)C] -TCB在各种脂肪酸组成的胶束中的溶解度。由单个脂肪酸组成的胶束与更长链长的那些脂肪酸相比,表现出更高的[(14)C] -TCB溶解度。同样,长链脂肪酸亚油酸的胶束比由等量的肉豆蔻酸(14:0),棕榈酸(16:0),硬脂酸(18: 0)或亚油酸(18:2)。与亚油酸胶束制剂相比,原位灌肠制剂中的[(14)C] -TCB(60μM)的系统生物利用度比亚油酸胶束中的肠释放高2.2倍。 vivo鱼在体内暴露于0.5或5.0 mg TCB / kg饲料10天后,导致原位肠道制剂中[(14)C] -TCB的后续全身生物利用度降低45%至47%。总肠细胞色素P450的含量不受TCB暴露的显着影响。仅在5.0 mg TCB / kg饮食治疗中发现了可免疫检测的CYP1A。对照组,0.5和5 mg TCB / kg饮食组相应的肠道芳基烃羟化酶(AHH)活性分别为2.46 +/- 1.16、2.43 +/- 1.58和11.35 +/- 10.25 pmol / min / mg蛋白。 。原位制备中的[(14)C] -TCB在单次通过fish鱼的肠粘膜时仅被小程度地代谢。高变异性和低代谢率排除了代谢量与饮食TCB预处理之间的联系。组织样品提取物的分析显示有4个次要峰,通过与2-OH-3,4,3',4'-TCB,4-OH-3,5,3', 4'-TCB和5-OH-3,4,3',4'-TCB。第四名仍然不明。在饮食剂量为5.0 mg TCB / kg时,肠的组织学变化(如粘膜下层变薄和杯状细胞数量增加)很明显。这些结果表明,TCB肠道的生物利用度可能与胶束组成以及TCB暴露史有关。此外,单程肠道代谢似乎对饮食TCB的生物转化修饰影响不大。

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