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Absorption, distribution, metabolism and excretion of selenium following oral administration of elemental selenium nanoparticles or selenite in rats

机译:大鼠口服元素硒纳米粒或亚硒酸盐后硒的吸收,分布,代谢和排泄

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摘要

A suspension of nanoparticles of BSA-stabilized red amorphous elemental selenium (Se) or an aqueous solution of sodium selenite was repeatedly administered by oral gavage for 28 days at 0.05 mg/kg bw/day (low dose) or at 0.5 mg/kg bw/day (high dose) as Se to female rats. Prior to administration, the size distribution of the Se nanoparticles was characterized by dynamic light scattering and transmission electron microscopy, which showed that the particles’ mean diameter was 19 nm and ranged in size from 10-80 nm. Following administration of the high dose of Se nanoparticles or selenite the concentration of Se was determined by ICP-MS in liver, kidney, urine, feces, stomach, lungs, plasma at µg/g level and in brain and muscle tissue at sub-µg/g level. In order to test if any elemental Se was present in liver, kidney or feces, an in situ derivatization selective to elemental Se was made by treatment with sulfite, which resulted in formation of the selenosulfate anion. This Se species was selectively and quantitatively determined by anion exchange HPLC with ICP-MS detection. The results showed that elemental Se was present in the livers, kidneys and feces from animals exposed to low and high doses of elemental Se nanoparticles or to selenite, and was detected also in the same samples from control animals. The fraction of Se present as elemental Se in livers and kidneys from the high dose animals was significantly larger than the similar fraction in samples from the low dose animals or from the controls. This suggested that the natural metabolic pathways of Se were exhausted when given the high dose of elemental Se or selenite resulting in a non-metabolized pool of elemental Se. Both dosage forms of Se were bioavailable as demonstrated by the blood biomarker selenoprotein P, which was equally up-regulated in the high-dose animals for both dosage forms of Se. Finally, the excretion of Se in urine and its occurrence as Se-methylseleno-N-Acetyl-galactosamine and trimethylselenonium-ion demonstrated that both dosage forms were metabolized and excreted. The results of the study showed that both forms of Se were equally absorbed, distributed, metabolized and excreted, but the detailed mechanism of the fate of the administered elemental Se or selenite in the gastro-intestinal tract of rats remains unclear.
机译:通过口服管饲法以0.05 mg / kg bw /天(低剂量)或0.5 mg / kg bw的剂量连续重复施用BSA稳定的红色非晶态硒(Se)纳米颗粒悬浮液或亚硒酸钠水溶液。 /日(高剂量)作为硒对雌性大鼠。给药前,通过动态光散射和透射电子显微镜对硒纳米粒子的尺寸分布进行了表征,结果表明该粒子的平均直径为19 nm,尺寸范围为10-80 nm。施用高剂量的硒纳米颗粒或亚硒酸盐后,通过ICP-MS测定肝脏,肾脏,尿液,粪便,胃,肺,血浆中微克/克的硒含量以及脑和肌肉组织中微克的硒含量/ g级。为了测试肝,肾或粪便中是否存在任何元素硒,通过亚硫酸盐处理对元素硒进行选择性的原位衍生化反应,从而形成硒代硫酸根阴离子。通过采用ICP-MS检测的阴离子交换HPLC有选择地和定量地确定了这种硒的种类。结果表明,暴露于低剂量和高剂量元素硒纳米颗粒或亚硒酸盐的动物的肝脏,肾脏和粪便中都存在元素硒,在对照动物的相同样品中也检测到了元素硒。高剂量动物在肝脏和肾脏中以元素硒形式存在的硒的比例显着大于低剂量动物或对照样品中硒的比例。这表明,当给予高剂量的元素硒或亚硒酸盐时,硒的自然代谢途径就被耗尽,从而导致元素硒的未代谢池。硒的两种剂型都是可生物利用的,如血液生物标记物硒蛋白P所证明的,硒蛋白的两种剂型在高剂量动物中均被上调。最后,尿中硒的排泄及其以硒-甲基硒代-N-乙酰基-半乳糖胺和三甲基硒代离子的出现表明两种剂型均被代谢和排泄。研究结果表明,两种形式的硒均被吸收,分布,代谢和排泄,但尚不清楚大鼠胃肠道中元素硒或亚硒酸盐施用的命运的详细机制。

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