Department of Toxicology, University of Würzburg, Versbacher Strasse 9, 97078, Würzburg, Germany.
Department of Inorganic Chemistry, University of Würzburg, Am Hubland, 97074, Würzburg, Germany.
Arch Toxicol. 2023 Dec;97(12):3095-3111. doi: 10.1007/s00204-023-03603-3. Epub 2023 Oct 4.
1,1,2-Trifluoroethene (HFO-1123) is anticipated for use as a refrigerant with low global warming potential. Inhalation studies on HFO-1123 in rats indicated a low potential for toxicity (NOAELs ≥ 20,000 ppm). In contrast, single inhalation exposure of Goettingen minipigs (≥ 500 ppm) and New Zealand white rabbits (≥ 1250 ppm) resulted in severe toxicity. It has been suggested that these pronounced species-differences in toxicity may be attributable to species-differences in biotransformation of HFO-1123 via the mercapturic acid pathway. Therefore, the overall objective of this study was to evaluate species-differences in glutathione (GSH) dependent in vitro metabolism of HFO-1123 in susceptible versus less susceptible species and humans as a basis for human risk assessment. Biotransformation of HFO-1123 to S-(1,1,2-trifluoroethyl)-L-glutathione (1123-GSH) and subsequent cysteine S-conjugate β-lyase-mediated cleavage of the corresponding cysteine conjugate (1123-CYS) was monitored in hepatic and renal subcellular fractions of mice, rats, minipigs, rabbits, and humans. While 1123-GSH formation occurred at higher rates in rat and rabbit liver S9 compared to minipig and human S9, increased β-lyase cleavage of 1123-CYS was observed in minipig kidney cytosol as compared to cytosolic fractions of other species. Increased β-lyase activity in minipig cytosol was accompanied by time-dependent formation of monofluoroacetic acid (MFA), a highly toxic compound that interferes with cellular energy production via inhibition of aconitase. Consistent with the significantly lower β-lyase activity in human cytosols, the intensity of the MFA signal in human cytosols was only a fraction of the signal obtained in minipig subcellular fractions. Even though the inconsistencies between GSH and β-lyase-dependent metabolism do not allow to draw a firm conclusion on the overall contribution of the mercapturic acid pathway to HFO-1123 biotransformation and toxicity in vivo, the β-lyase data suggest that humans may be less susceptible to HFO-1123 toxicity compared to minipigs.
1,1,2-三氟乙烯(HFO-1123)有望作为一种全球变暖潜能值较低的制冷剂使用。大鼠吸入 HFO-1123 的研究表明其毒性较低(NOAELs≥20000ppm)。相比之下,哥廷根小型猪(≥500ppm)和新西兰白兔(≥1250ppm)单次吸入暴露会导致严重毒性。有人认为,这些明显的物种间毒性差异可能归因于 HFO-1123 通过巯基尿酸途径的生物转化的物种差异。因此,本研究的总体目标是评估易感和不易感物种以及人类中 GSH 依赖性 HFO-1123 体外代谢的物种差异,作为人类风险评估的基础。监测了 HFO-1123 向 S-(1,1,2-三氟乙基)-L-谷胱甘肽(1123-GSH)的生物转化以及随后胱氨酸 S-结合物β-裂合酶对相应胱氨酸结合物(1123-CYS)的切割在小鼠、大鼠、小型猪、兔子和人类的肝和肾亚细胞部分中进行。虽然大鼠和兔肝 S9 中 1123-GSH 的形成速率高于小型猪和人 S9,但与其他物种的细胞溶质部分相比,小型猪肾细胞溶质中 1123-CYS 的β-裂合酶切割增加。在小型猪细胞溶质中β-裂合酶活性增加的同时,形成了单氟乙酸(MFA),这是一种高度毒性的化合物,通过抑制乌头酸酶干扰细胞能量产生。与人类细胞溶质中β-裂合酶活性显著降低一致,人类细胞溶质中 MFA 信号的强度仅是小型猪亚细胞部分获得信号的一小部分。尽管 GSH 和β-裂合酶依赖性代谢之间的不一致不允许对巯基尿酸途径对 HFO-1123 生物转化和体内毒性的总体贡献得出明确结论,但β-裂合酶数据表明,与小型猪相比,人类可能对 HFO-1123 毒性的敏感性较低。
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