Sauer J M, Smith R L, Bao J, Kattnig M J, Kuester R K, McClure T D, Mayersohn M, Sipes I G
Department of Pharmacology and Toxicology, College of Pharmacy, University of Arizona, Tucson 85721-0207, USA.
Drug Metab Dispos. 1997 Jun;25(6):732-9.
trans-Methyl styryl ketone (MSK; trans-4-phenyl-3-buten-2-one) is a beta-unsaturated ketone that has a wide range of uses in industry and is present in numerous consumer products. Although MSK has been shown to be positive in several in vitro mutagenic assays, it does not seem to be overtly toxic in animal models. This lack of toxicity may relate to its poor absorption and/or rapid elimination. However, little is known about the fate of MSK in the body. Studies were conducted to characterize the absorption, and disposition kinetics of MSK after intravenous, oral, and topical administration to male Fischer 344 rats. After intravenous administration of [14C]MSK (20 mg/kg, 120 microCi/kg), blood concentration-time data could be characterized with a biexponential equation and apparent first-order elimination kinetics. The following pharmacokinetic parameter values were obtained (mean +/- SD): terminal disposition half-life, 17.7 +/- 0.08 min; apparent steady-state volume of distribution, 0.89 +/- 0.14 liters/kg; systemic body clearance, 68.9 +/- 10.0 ml/kg *min; and mean residence time, 13.1 +/- 2.2 min. Within 48 hr, 95.5% of the dose was excreted in the urine and 2.7% in the feces. The major blood metabolite after intravenous administration was identified by GC/MS as the 4-phenyl-3-buten-2-ol (methyl styryl carbinol). After oral administration of [14C]MSK (200 mg/kg, 100 microCI/kg), approximately 96.6% of the dosed radioactivity was recovered in the urine and 4.8% in the faces within 48 hr. Major urinary metabolites identified by LC-MS/MS and quantified by HPLC radioassay were N-phenylacetyl-L-glycine (64.9% of dose) and N-benzyl-L-glycine (9.9% of dose). Parent compound could not be detected in the blood after oral administration, and 14C-equivalents in the blood never exceeded 1.3% of the dose. Results suggest near-total presystemic elimination of the oral dose. After topical application of [14C]MSK (250 mg/kg, 50 microCi/kg), > 60% of the dose was absorbed, and the majority of the dose was excreted into the urine (55% of dose) in the form of metabolites. Urinary metabolites were similar to those described after oral administration. 14C-equivalents were not detected in the blood at any time after topical administration. These results indicate that MSK is almost totally metabolized before systemic distribution after oral or topical administration. The systemic exposure dose of MSK seems to be exceedingly low at the doses studied herein.
反式甲基苯乙烯基酮(MSK;反式-4-苯基-3-丁烯-2-酮)是一种β-不饱和酮,在工业上有广泛用途,且存在于众多消费品中。尽管MSK在多种体外诱变试验中呈阳性,但在动物模型中似乎并无明显毒性。这种缺乏毒性的情况可能与其吸收不良和/或快速消除有关。然而,人们对MSK在体内的代谢情况知之甚少。本研究旨在对雄性Fischer 344大鼠静脉内、口服和局部给药后MSK的吸收和处置动力学进行表征。静脉注射[14C]MSK(20 mg/kg,120 μCi/kg)后,血药浓度-时间数据可用双指数方程和表观一级消除动力学进行表征。获得以下药代动力学参数值(平均值±标准差):终末处置半衰期,17.7±0.08分钟;表观稳态分布容积,0.89±0.14升/千克;全身清除率,68.9±10.0毫升/千克·分钟;平均驻留时间,13.1±2.2分钟。在48小时内,95.5%的剂量经尿液排泄,2.7%经粪便排泄。静脉给药后的主要血液代谢产物经气相色谱/质谱法鉴定为4-苯基-3-丁烯-2-醇(甲基苯乙烯基甲醇)。口服[14C]MSK(200 mg/kg,100 μCi/kg)后,在48小时内约96.6%的给药放射性在尿液中回收,4.8%在粪便中回收。经液相色谱-串联质谱法鉴定并通过高效液相色谱放射性测定法定量的主要尿液代谢产物为N-苯基乙酰-L-甘氨酸(占剂量的64.9%)和N-苄基-L-甘氨酸(占剂量的9.9%)。口服给药后血液中未检测到母体化合物,血液中的14C等效物从未超过剂量的1.3%。结果表明口服剂量几乎完全在体循环前消除。局部应用[14C]MSK(250 mg/kg,50 μCi/kg)后,>60%的剂量被吸收,且大部分剂量以代谢产物的形式经尿液排泄(占剂量的55%)。尿液代谢产物与口服给药后描述的相似。局部给药后任何时间血液中均未检测到14C等效物。这些结果表明,MSK在口服或局部给药后全身分布前几乎完全代谢。在本文研究的剂量下,MSK的全身暴露剂量似乎极低。
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