氯菊酯类杀虫剂联苯菊酯在长 Evans 大鼠体内的组织时间进程及生物利用度
Tissue time course and bioavailability of the pyrethroid insecticide bifenthrin in the Long-Evans rat.
作者信息
Hughes Michael F, Ross David G, Edwards Brenda C, DeVito Michael J, Starr James M
机构信息
a U.S. Environmental Protection Agency, Office of Research and Development, National Health and Environmental Effects Research Laboratory, Research Triangle Park , NC , USA .
b National Toxicology Program, National Institute of Environmental Health Sciences, Research Triangle Park , NC , USA , and.
出版信息
Xenobiotica. 2016;46(5):430-8. doi: 10.3109/00498254.2015.1081710. Epub 2015 Sep 14.
1. Pyrethroids are neurotoxic and parent pyrethroid appears to be toxic entity. This study evaluated the oral disposition and bioavailability of bifenthrin in the adult male Long-Evans rat. 2. In the disposition study, rats were administered bifenthrin (0.3 or 3 mg/kg) by oral gavage and serially sacrificed (0.25 h to 21 days). Blood, liver, brain and adipose tissue were removed. In the bioavailability study, blood was collected serially from jugular vein cannulated rats (0.25 to 24 h) following oral (0.3 or 3 mg/kg) or intravenous (0.3 mg/kg) administration of bifenthrin. Tissues were extracted and analyzed for bifenthrin by high-performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS). 3. Bifenthrin concentration in blood and liver peaked 1-2-h postoral administration and were approximately 90 ng/ml (or g) and 1000 ng/ml (or g) for both tissues at 0.3 and 3 mg/kg, respectively. Bifenthrin was rapidly cleared from both blood and liver. Brain concentrations peaked at 4-6 h and were lower than in blood at both doses (12 and 143 ng/g). Bifenthrin in adipose tissue peaked at the collected time points of 8 (157 ng/g) and 24 (1145 ng/g) h for the 0.3 and 3 mg/kg doses, respectively and was retained 21 days postoral administration. Following intravenous administration, the blood bifenthrin concentration decreased bi-exponentially, with a distribution half-life of 0.2 h and an elimination half-life of 8 h. Bifenthrin bioavailability was approximately 30%. These disposition and kinetic bifenthrin data may decrease uncertainties in the risk assessment for this pyrethroid insecticide.
- 拟除虫菊酯具有神经毒性,母体拟除虫菊酯似乎是毒性实体。本研究评估了联苯菊酯在成年雄性长 Evans 大鼠体内的口服处置情况和生物利用度。2. 在处置研究中,通过口服灌胃给大鼠施用联苯菊酯(0.3 或 3mg/kg),并按顺序处死(0.25 小时至 21 天)。采集血液、肝脏、大脑和脂肪组织。在生物利用度研究中,在口服(0.3 或 3mg/kg)或静脉注射(0.3mg/kg)联苯菊酯后,从颈静脉插管的大鼠中按顺序采集血液(0.25 至 24 小时)。通过高效液相色谱 - 串联质谱法(HPLC-MS/MS)提取并分析组织中的联苯菊酯。3. 口服给药后 1 - 2 小时,血液和肝脏中联苯菊酯浓度达到峰值,在 0.3mg/kg 和 3mg/kg 剂量下,两种组织的浓度分别约为 90ng/ml(或 g)和 1000ng/ml(或 g)。联苯菊酯从血液和肝脏中迅速清除。大脑浓度在 4 - 6 小时达到峰值,且在两个剂量下均低于血液中的浓度(12 和 143ng/g)。在 0.3mg/kg 和 3mg/kg 剂量下,脂肪组织中联苯菊酯分别在 8 小时(157ng/g)和 24 小时(1145ng/g)的采集时间点达到峰值,并在口服给药后 21 天内持续存在。静脉注射后,血液中联苯菊酯浓度呈双指数下降,分布半衰期为 0.2 小时,消除半衰期为 8 小时。联苯菊酯的生物利用度约为 30%。这些联苯菊酯的处置和动力学数据可能会降低这种拟除虫菊酯类杀虫剂风险评估中的不确定性。
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