含硫醇螯合剂对六价铬致小鼠肝损伤的保护作用。

S Ueno
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摘要

研究了l-半胱氨酸乙酯(LCEE)、l-半胱氨酸甲酯(LCME)、N-乙酰基- l-(+)-半胱氨酸(NAC)、2,3-二巯基-1-丙磺酸(DMPS)、N-(2-巯基丙酰)-甘氨酸(MPG)、2,3-二巯基琥珀酸(DMSA)等螯合剂对六价铬在雄性小鼠体内的分布、排泄和肝毒性的影响。螯合剂(500 mg/kg)单次静脉注射,或在重铬酸钾(20 mg Cr/kg)作为六价铬给药后30分钟静脉注射。在给药后立即注射螯合剂,LCEE、LCME、NAC、DMPS和MPG降低肝脏和肾脏中的铬含量,促进尿中铬的排泄。以血清鸟氨酸氨基甲酰转移酶(OCT)活性评价,LCEE、LCME、DMPS和MPG对铬所致肝损伤有明显的预防作用。另一方面,在给铬后30min注射这些螯合剂时,只有DMSA可以预防金属引起的肝损伤,并降低肝脏中铬的含量。然而,当金属给药后3小时给予DMSA时,对它们没有治疗效果。这些结果表明,所测试的螯合剂可用于治疗六价铬中毒,但由于给予金属后的时间间隔,螯合剂的治疗效果存在差异。
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Protective effects of thiol containing chelating agents against liver injury induced by hexavalent chromium in mice.

The effects of the chelating agents, L-cysteine ethyl ester (LCEE), L-cysteine methyl ester (LCME), N-acetyl-L-(+)-cysteine (NAC), 2,3-dimercapto-1-propanesulfonic acid (DMPS), N-(2-mercaptopropionyl)-glycine (MPG), and 2,3-dimercaptosuccinic acid (DMSA), on the distribution, excretion and hepatotoxicity of ip injected hexavalent chromium were studied in male mice. The chelating agents (500 mg/kg) were injected iv as single doses given immediately or 30 min after potassium dichromate (20 mg Cr/kg) as hexavalent chromium was administered. When the chelating agents were injected immediately after the metal compound was administered, LCEE, LCME, NAC, DMPS, and MPG reduced the chromium contents in the liver and kidney, and facilitated the urinary excretion of chromium. The liver injury induced by chromium, which was evaluated by serum ornithine carbamyl transferase (OCT) activity, was prevented significantly by LCEE, LCME, DMPS, and MPG. On the other hand, when these chelating agents were injected at 30 min after the chromium administration, only DMSA could prevent the liver injury induced by the metal, and decreased the chromium contents in the liver. However, when DMSA was given at 3 hr after the metal administration, there was no therapeutic effect on them. These results suggest that the chelating agents tested may be useful in the treatment of intoxications due to hexavalent chromium, but there is the difference in the therapeutic effects of the chelating agents owing to the time intervals after the administration of the metal.

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