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重铬酸钠的肾毒性取决于给药途径。

Nephrotoxicity of sodium dichromate depending on the route of administration.

作者信息

Kim E, Na K J

机构信息

Korea Ginseng and Tobacco Research Institute, Taejon.

出版信息

Arch Toxicol. 1991;65(7):537-41. doi: 10.1007/BF01973713.

Abstract

A comparison of the effects of intraperitoneal and subcutaneous routes of administration of sodium dichromate on nephrotoxicity in rats was studied. Dichromate when injected subcutaneously (SC group) produced a higher degree of nephrotoxicity than when administered intraperitoneally (IP group). It caused severe progressive proteinuria followed by polyuria and glucosuria, reaching maximum levels at 3 days after treatment in the SC group, whereas it produced mild proteinuria without glucosuria in the IP group. The dose-dependent increases in blood urea nitrogen (BUN) and creatinine concentrations, shown in the SC group, were not observed in the IP group. However, between the two groups, there were no great differences in either the urinary excretion rate of chromium or the electrophoretic patterns of urinary protein in the day 1 urine specimens. Pretreatment of phenobarbital (PB) had no remarkable effect on the dichromate-induced nephrotoxicity. In contrast, it potentiated dichromate-induced hepatotoxicity, the indices of which were the elevation in serum alanine aminotransferase (ALT) activity and hepatic lipid peroxide formation. These results suggest that the dependence of dichromate-induced nephrotoxicity on the route of administration is related to the chemical forms of chromium reaching the kidney, and the necrotizing property of dichromate results from its metabolic fate in vivo.

摘要

研究了腹腔注射和皮下注射重铬酸钠对大鼠肾毒性影响的比较。重铬酸盐皮下注射(SC组)时产生的肾毒性程度高于腹腔注射(IP组)。它导致严重的进行性蛋白尿,随后出现多尿和糖尿,在SC组中治疗后3天达到最高水平,而在IP组中产生轻度蛋白尿且无糖尿。SC组中出现的血尿素氮(BUN)和肌酐浓度的剂量依赖性增加在IP组中未观察到。然而,两组之间,第1天尿液标本中铬的尿排泄率或尿蛋白的电泳图谱均无显著差异。苯巴比妥(PB)预处理对重铬酸盐诱导的肾毒性无显著影响。相反,它增强了重铬酸盐诱导的肝毒性,其指标是血清丙氨酸转氨酶(ALT)活性升高和肝脂质过氧化物形成。这些结果表明,重铬酸盐诱导的肾毒性对给药途径的依赖性与到达肾脏的铬的化学形式有关,重铬酸盐的坏死特性源于其在体内的代谢命运。

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