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口服磺胺二甲嘧啶对Fischer 344大鼠甲状腺激素水平的影响。

Influence of oral administration of sulfamethazine on thyroid hormone levels in Fischer 344 rats.

作者信息

Fullerton F R, Kushmaul R J, Suber R L, Littlefield N A

机构信息

Department of Health and Human Services, National Center for Toxicological Research, Jefferson, Arkansas 72079.

出版信息

J Toxicol Environ Health. 1987;22(2):175-85. doi: 10.1080/15287398709531061.

Abstract

Fischer 344 rats (810 of each sex) were divided into treatment groups and fed diets containing 0, 10, 40, 600, 1200, or 2400 ppm sulfamethazine. Serum samples were analyzed for levels of thyroid-stimulating hormone (TSH), total thyroxine (T4), total triiodothyronine (T3), and T3 uptake after 12, 18, or 24 mo of continuous dosing. There were no statistically significant differences in T3 levels or percent T3 uptake for either sex after any of the exposure periods. The serum T4 levels were lower (p less than 0.05) for females dosed at 1200 and 2400 ppm for 18 mo and for males dosed at 600, 1200, or 2400 ppm sulfamethazine for 24 mo than for those dosed at levels of 40 ppm or less. Serum TSH levels showed a general increasing trend (but not statistically significant) among animals receiving 600 ppm or more sulfamethazine. There was a significant dose-related reduction in (T3 + T4)/TSH ratio for both sexes (p less than 0.05) after 18 and 24 mo of exposure at dose levels of 600 ppm or more. A lack of response at 12 mo may have been due to the shorter treatment time. At each sacrifice period both sexes of rats fed sulfamethazine at 1200 and 2400 ppm had significantly heavier (p less than 0.05) thyroid weights than animals fed control diet. The heavier thyroid weights in the dosed animals may have resulted from increased TSH levels. The cause of reduction in serum T4 was not clearly evident. Therefore, the thyroid hormone to pituitary feedback mechanism apparently compensated for sulfamethazine effects in most animals. This would suggest that the thyroid gland was not irreversibly affected.

摘要

将810只雄性和810只雌性Fischer 344大鼠分为不同处理组,分别喂食含0、10、40、600、1200或2400 ppm磺胺二甲嘧啶的日粮。连续给药12、18或24个月后,分析血清样本中促甲状腺激素(TSH)、总甲状腺素(T4)、总三碘甲状腺原氨酸(T3)水平以及T3摄取率。在任何暴露期后,两性的T3水平或T3摄取百分比均无统计学显著差异。在18个月时,喂食1200和2400 ppm的雌性大鼠血清T4水平较低(p<0.05);在24个月时,喂食600、1200或2400 ppm磺胺二甲嘧啶的雄性大鼠血清T4水平低于喂食40 ppm及以下的大鼠。在接受600 ppm及以上磺胺二甲嘧啶的动物中,血清TSH水平总体呈上升趋势(但无统计学显著性)。在剂量水平为600 ppm及以上暴露18和24个月后,两性的(T3+T4)/TSH比值均出现显著的剂量相关降低(p<0.05)。12个月时无反应可能是由于治疗时间较短。在每个处死期,喂食1200和2400 ppm磺胺二甲嘧啶的大鼠两性甲状腺重量均显著重于喂食对照日粮的动物(p<0.05)。给药动物甲状腺较重可能是由于TSH水平升高所致。血清T4降低的原因尚不清楚。因此,甲状腺激素对垂体的反馈机制显然在大多数动物中补偿了磺胺二甲嘧啶的作用。这表明甲状腺未受到不可逆的影响。

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