给药载体对大鼠CCl4肝毒性和CHCl3肾毒性的影响。

P Raymond, G L Plaa
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引用次数: 10

摘要

关于灌胃剂、玉米油(CO)和水悬浮液对卤代烷毒性的影响,文献中有相互矛盾的结果。本研究的目的是评估口服给药载体对CCl4急性肝毒性和CHCl3肾毒性的影响。用玉米油(CO)或乳剂(EL620)或Tween-85 (Tw-85)的5%水溶液(10 ml/kg)给雄性sd大鼠单剂量CCl4或CHCl3处理(po)。治疗后48 h处死大鼠。取血测定血浆丙氨酸转氨酶(ALT),取肾皮质片测定对氨基马尿酸(PAH)掺入。不同灌胃组剂量-反应曲线的斜率和ED50的比较,虽然没有显著差异,但表明CO对CHCl3肾毒性的效力明显增强,而对CCl4肝毒性则没有增强的趋势。然而,衡量CCl4影响严重程度的ALT值也表明,与EL620和Tw-85相比,CO倾向于在低毒性发生率下增强CCl4肝毒性。此外,在高剂量下,CO明显增强了CHCl3肾毒性效应的严重程度,通过切片与中PAH比率来测量。当以一氧化碳给药时,暴露于这些化学物质所产生的更严重的损害,与观察到的它们的效力趋势(剂量-反应曲线)是一致的。我们的结果与文献中报道的灌胃CO增加卤代烷的毒性一致。因此,在肝和肾毒性试验中,一氧化碳应被视为潜在的混杂因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of dosing vehicle on the hepatotoxicity of CCl4 and nephrotoxicity of CHCl3 in rats.
There are conflicting results in the literature concerning the effect of gavage vehicle, corn oil (CO) versus aqueous suspension, on the toxicity of haloalkanes. The purpose of our study was to assess the influence of oral dosing vehicle on the acute hepatotoxicity of CCl4 and nephrotoxicity of CHCl3. Male Sprague-Dawley rats, fed ad libitum, were treated (po) with single doses of CCl4 or CHCl3 using corn oil (CO), or an aqueous preparation (5%) of Emulphor (EL620) or Tween-85 (Tw-85) as vehicle (10 ml/kg). Rats were killed 48 h after treatment. Blood was collected for plasma alanine aminotransferase (ALT) determination and renal cortical slices were prepared for p-aminohippuric acid (PAH) incorporation. The comparison, between gavage vehicles, of the slopes and ED50 of the dose-response curves, although not significantly different, indicated clear trends for enhanced potency with CO for CHCl3 nephrotoxicity but not for CCl4 hepatotoxicity. However, ALT values, a measure of the severity of effect for CCl4, also indicated that CO, when compared to EL620 and Tw-85, tended to enhance CCl4 hepatotoxicity at low toxicity incidence. Furthermore, CO clearly enhanced the severity of effect for CHCl3 nephrotoxicity, as measured by the slice-to-medium PAH ratios, at high dosage. The greater severity of the lesion produced by exposure to these chemicals, when administered in CO, is consistent with the trends observed for their potency (dose-response curves). Our results agree with an increased toxicity of haloalkanes by the gavage vehicle CO reported in the literature. Thus, CO should be considered a potential confounder in hepato- and nephrotoxicity assays.
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