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2,3,3,3-四氟丙烯(HFO-1234yf)的急性、发育、遗传和吸入毒理学。

The acute, developmental, genetic and inhalation toxicology of 2,3,3,3-tetrafluoropropene (HFO-1234yf).

机构信息

Honeywell International, Morristown, NJ 07962-1139, USA.

出版信息

Drug Chem Toxicol. 2013 Oct;36(4):412-20. doi: 10.3109/01480545.2012.749273. Epub 2013 Jun 6.

DOI:10.3109/01480545.2012.749273
PMID:23742174
Abstract

2,3,3,3-Tetrafluoropropene (HFO-1234yf) is being developed as a refrigerant because it has a very low global warming potential (less than 10), as contrasted to the hydrofluorocarbons, which is intended to replace with values of over 500. Several toxicology studies were conducted to develop a toxicology profile for this material. There was no lethality in mice and rats receiving single 4-hour exposures up to 101,850 or 405,800 ppm, respectively. Additionally, there was no mortality or clinical signs of toxicity when rabbits were exposed to 100,000 ppm for 1 hour. Exposures up to 120,000 ppm did not induce cardiac sensitization to adrenalin in dogs. Rats were exposed to HFO-1234yf at levels of 5000, 20,000 and 50,000 ppm 6 hours/day 5 days/week for 2 weeks and at levels of 5000, 15,000 and 50,000 ppm for 4 weeks and for 90 days. No treatment-related adverse effects were noted in these studies. HFO-1234yf was not genotoxic in a mouse and a rat micronucleus assay, and unscheduled DNA synthesis assay and was not clastogenic in human lymphocytes. HFO-1234yf was mutagenic to Salmonella typhimurium TA 100 and Escherichia coli (WP2 uvrA) at concentrations of 20% and higher in the presence of metabolic activation only. There were no biologically significant effects in a rat developmental toxicity study with exposures up to 50,000 ppm.

摘要

2,3,3,3-四氟丙烯(HFO-1234yf)正被开发为一种制冷剂,因为它的全球变暖潜能值(GWP)非常低(不到 10),与氢氟碳化物相比,氢氟碳化物的 GWP 值超过 500,旨在取代 HFO-1234yf。进行了几项毒理学研究,以为此材料开发毒理学概况。在分别接受高达 101,850 或 405,800 ppm 的单次 4 小时暴露后,小鼠和大鼠均无致死性。此外,当兔子暴露于 100,000 ppm 1 小时时,没有死亡或毒性的临床症状。在狗身上,暴露于高达 120,000 ppm 不会引起肾上腺素对心脏的敏感化。大鼠在 5000、20000 和 50000 ppm 下暴露 6 小时/天,5 天/周,持续 2 周,在 5000、15000 和 50000 ppm 下暴露 4 周和 90 天。在这些研究中,没有观察到与治疗相关的不良反应。在小鼠和大鼠微核试验、非计划 DNA 合成试验中,HFO-1234yf 未显示遗传毒性,在人淋巴细胞中也未显示出致裂性。在存在代谢激活的情况下,HFO-1234yf 对鼠伤寒沙门氏菌 TA 100 和大肠杆菌(WP2 uvrA)的致突变性仅在 20%及以上浓度时才有。在暴露于高达 50000 ppm 的大鼠发育毒性研究中,没有生物学意义上的影响。

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