National Research Council, Washington, DC 20001, United States.
Neurotoxicology. 2012 Jun;33(3):332-46. doi: 10.1016/j.neuro.2012.02.006. Epub 2012 Feb 14.
Previously, we reported that acute treatment with propoxur or carbaryl decreased the duration of the photic after discharge (PhAD) of flash evoked potentials (FEPs). In the current studies, we compared the effects of acute or repeated exposure to a mixture of carbaryl and propoxur (1:1.45 ratio; propoxur:carbaryl) on the duration of the PhAD and brain ChE activity in Long Evans rats. Animals were exposed (po) either to a single dose (0, 3, 10, 45 or 75 mg/kg), or 14 daily dosages (0, 3, 10, 30, 45 mg/kg), of the mixture. Acute and repeated treatment with 3mg/kg (or greater) of the mixture produced dose-related inhibition of brain ChE activity. Compared to controls, the PhAD duration decreased after acute administration of 75 mg/kg or repeated treatment with 30 mg/kg of the mixture. The linear relationship between the percent of control brain ChE activity and the PhAD duration was similar for both exposure paradigms. Dose-response models for the acute and repeated exposure data did not differ for brain ChE activity or the duration of the PhAD. Repeated treatment with the mixture resulted in slightly less (13-22%) erythrocyte ChE inhibition than acute exposure. Both acute and repeated treatment resulted in dose-additive results for the PhAD duration and less than dose-additive responses (6-16%) for brain ChE activity for the middle range of dosages. Acute treatment resulted in greater than dose-additive erythrocyte ChE inhibition (15-18%) at the highest dosages. In contrast, repeated treatment resulted in less than dose-additive erythrocyte ChE inhibition (16-22%) at the middle dosages. Brain and plasma levels of propoxur and carbaryl did not differ between the acute and repeated dosing paradigms. In summary, a physiological measure of central nervous system function and brain ChE activity had similar responses after acute or repeated treatment with the carbamate mixture, and brain ChE showed only small deviations from dose-additivity. Erythrocyte ChE activity had larger differences between the acute and repeated treatment paradigms, and showed slightly greater deviations from dose-additivity. Because these treatments utilized larger dosages than anticipated environmental exposures, concern for non-additive effects in humans is minimized. The small magnitude of the deviations from dose-additivity also suggest that in the absence of repeated exposure data, results from an acute study of readily reversible carbamate toxicity can be used to estimate the response to repeated daily exposures.
此前,我们报道急性处理敌百虫或西维因会缩短闪光诱发电位(FEPs)的光后放电(PhAD)持续时间。在当前的研究中,我们比较了急性或重复接触敌百虫和西维因混合物(比例为 1:1.45;敌百虫:西维因)对 Long Evans 大鼠 PhAD 持续时间和脑 ChE 活性的影响。动物经口(po)暴露于单剂量(0、3、10、45 或 75mg/kg)或 14 个每日剂量(0、3、10、30、45mg/kg)的混合物。急性和重复处理 3mg/kg(或更高)的混合物会导致脑 ChE 活性的剂量相关抑制。与对照组相比,混合物的急性给药 75mg/kg 或重复治疗 30mg/kg 后,PhAD 持续时间缩短。暴露模式下的脑 ChE 活性与 PhAD 持续时间的百分比之间的线性关系相似。急性和重复暴露数据的剂量-反应模型对于脑 ChE 活性或 PhAD 持续时间没有差异。与急性暴露相比,混合物的重复处理导致红细胞 ChE 抑制减少(13-22%)。急性和重复处理均导致 PhAD 持续时间和中剂量脑 ChE 活性的加和结果,而中间范围的剂量则导致低于加和的反应(6-16%)。急性处理在最高剂量下导致红细胞 ChE 抑制(15-18%)大于加和。相比之下,重复处理在中间剂量下导致红细胞 ChE 抑制(16-22%)低于加和。急性和重复给药方案之间,脑和血浆中的敌百虫和西维因水平没有差异。总之,中枢神经系统功能的生理测量和脑 ChE 活性在急性或重复接触氨基甲酸酯混合物后有相似的反应,脑 ChE 仅显示出与剂量相加性的微小偏差。红细胞 ChE 活性在急性和重复处理方案之间存在较大差异,且表现出略微偏离剂量相加性。由于这些处理方法使用了比预期环境暴露更大的剂量,因此人类对非加性效应的担忧最小化。剂量相加性偏差的幅度较小也表明,在没有重复暴露数据的情况下,急性研究中氨基甲酸酯毒性的可逆性结果可用于估计对每日重复暴露的反应。
