口服不同铝化合物对小鼠铝组织分布及组织中必需元素浓度的影响。

M Długaszek, M A Fiejka, A Graczyk, J C Aleksandrowicz, M Slowikowska
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引用次数: 20

摘要

为了评估胃肠道长期铝暴露的风险,研究了组织中铝的分布和以下基本元素:Ca, Mg, Zn, Cu和Fe的水平。铝以氯化铝、二羟铝碳酸钠或氢氧化铝的形式加入饮用水。小鼠(品系Pzh:SFIS)长期暴露于总剂量为700 mg的Al(每种Al化合物n = 15)。用原子吸收光谱法测定胃、肾、骨、肝中Al、Ca、Mg、Zn、Cu、Fe的浓度。AlCl3处理后,铝在所有被试组织中均有蓄积。与对照组中这些元素的浓度相比,肝脏中的铁浓度和肾脏中的锌浓度显著降低。在Al(OH)3处理组,只观察到骨中铝的积累,胃中铁浓度下降,肝和肾中铜浓度下降。NaAl(OH) 2co3处理组骨中Al浓度显著升高;检查组织中必需元素的浓度没有变化。除骨外,观察到的铝积累不伴有Ca和Mg浓度的变化。本研究表明,口服给药作为铝暴露的一种途径,可导致组织中铝的分散积累,其浓度取决于化学形式。
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Effects of various aluminium compounds given orally to mice on Al tissue distribution and tissue concentrations of essential elements.

To evaluate the risk of gastrointestinal long-term aluminium (Al) exposure, aluminium distribution and the levels of the following essential elements: Ca, Mg, Zn, Cu, and Fe in tissue were studied. Aluminium was administered in drinking water as aluminium chloride, dihydroxyaluminium sodium carbonate or aluminium hydroxide. Mice (strain Pzh:SFIS) were exposed to a total dose of 700 mg Al in long-term treatment (for each Al compound n = 15). Concentrations of Al, Ca, Mg, Zn, Cu, and Fe in stomach, kidneys, bone and liver were analyzed by atomic absorption spectrometry. After AlCl3 treatment, aluminium was found to accumulate in all tested tissues. A significant decrease in Fe concentration in liver and Zn in kidneys was observed in comparison to concentrations of these elements in the control group. In the Al(OH)3-treated group, accumulation of aluminium was observed in bone only and decline of Fe concentration in stomach and Cu in liver and kidney. In the NaAl(OH)2CO3-treated group the increase in Al concentration was significant in bone; there was no change in concentration of essential elements in the examined tissues. The observed aluminium accumulation was not accompanied by changes in Ca and Mg concentration except for bone. This study showed that oral administration as a route of Al exposure can result in diverging accumulation of aluminium in tissues, the concentration depending on the chemical form.

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