Saghir Shakil A, Lebofsky Margitta, Pinson David M, Rozman Karl K
Department of Pharmacology, Toxicology, and Therapeutics, University of Kansas Medical Center, 3901 Rainbow Blvd., Mail Stop 1018, Kansas City, KS 66160-7417, USA.
Toxicology. 2005 Nov 5;215(1-2):48-56. doi: 10.1016/j.tox.2005.06.009. Epub 2005 Aug 1.
Haber's Rule and associated time to coma after monochloroacetic acid (MCA) exposure in male Sprague-Dawley (SD) rats and time to death after 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) exposure in female Sprague-Dawley rats and male A/J mice were investigated at isoeffective or nearly isoeffective doses. Animals exposed to MCA received either single bolus intravenous (iv) doses or a loading dose rate via the iv route followed by a maintenance dose rate through subcutaneously implanted osmotic mini pumps. For TCDD, rats received a loading dose rate via bolus oral gavage followed by maintenance dose rates through iv injection every fourth day until death. Mice received both loading and maintenance (once a week) dose rates via oral gavage. Different dosing regimens were employed to demonstrate that the key to Haber's Rule lies not in the route of administration but in conducting experiments under conditions of kinetic steady state. Single doses of MCA produced inconsistent time responses but a reasonably constant c x t product (7657+/-391 mg/kg x min) which was not anticipated although it should have been expected because MCA's elimination half-life (2 h) is twice as long as its time to coma ( approximately 1h). Generation of kinetic steady state by infusion of MCA after iv injection of a loading dose rate resulted in a consistently decreasing time response with increasing dose which diminished the variability in the c x t (dose x time)=k relationship (8032+/-136 mg/kg x min). Both acute and chronic toxicity of TCDD under conditions of kinetic steady state yielded consistent time responses with inverse proportionality between dose and time leading to robust c x t=k products in both rats (1060+/-82 microg/kg x day) and mice (80+/-2 mg/kg x day).
研究了哈伯法则以及雄性斯普拉格-道利(SD)大鼠暴露于一氯乙酸(MCA)后昏迷时间、雌性斯普拉格-道利大鼠和雄性A/J小鼠暴露于2,3,7,8-四氯二苯并-对-二恶英(TCDD)后死亡时间,均采用等效应或接近等效应剂量。暴露于MCA的动物接受单次静脉推注剂量,或通过静脉途径给予负荷剂量率,随后通过皮下植入的渗透微型泵给予维持剂量率。对于TCDD,大鼠通过单次口服灌胃给予负荷剂量率,随后每四天通过静脉注射给予维持剂量率直至死亡。小鼠通过口服灌胃接受负荷剂量率和维持剂量率(每周一次)。采用不同的给药方案以证明哈伯法则的关键不在于给药途径,而在于在动力学稳态条件下进行实验。单次剂量的MCA产生的时间反应不一致,但c×t乘积(7657±391mg/kg·min)相当恒定,这虽然本应预期到(因为MCA的消除半衰期为2小时,是其昏迷时间(约1小时)的两倍),但却未被预期到。静脉注射负荷剂量率后通过输注MCA产生动力学稳态,导致随着剂量增加时间反应持续降低,这减少了c×t(剂量×时间)=k关系中的变异性(8032±136mg/kg·min)。在动力学稳态条件下,TCDD的急性和慢性毒性均产生一致的时间反应,剂量与时间呈反比,导致大鼠(1060±82μg/kg·天)和小鼠(80±2mg/kg·天)的c×t=k乘积均很稳定。
