Evaluation of Liver Toxicity of Neonates Following Intragastric Administration or Intratracheal Instillation of Polyethylene Microplatics to Pregnant Mice

G. Kim, Changyul Kim
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Abstract

ABSTRACT Background: Current research suggests that humans are exposed to microplastics through consumption of foods and beverages, the airway route, and a variety of other means. Objectives: We evaluated oxidative stress and inflammation from polyethylene microplastics (PE-MPs) in the neonatal liver through intragastric administration or intratracheal instillation in pregnant mice. Methods: PE-MPs were administered from gestational day 9 to postnatal day 7. The intragastric administration group (0.01 mg/mouse/day or 0.1 mg/mouse/day) and intratracheal instillation group (6 μ g/mouse/day or 60 μ g/mouse/day) of PE-MPs were administered. After sacrifice, the oxidative stress and inflammation of the neonatal livers were measured. Results: As a result of the oxidative stress caused by PE-MPs in the neonatal livers, glutathione peroxidase decreased in a concentration-dependent manner in the intragastric administration group compared to the control group and intratracheal instillation decreased in high concentration PE-MPs. The catalase level increased at high concentrations of intragastric administration and intratracheal instillation. To confirm the level of inflammation caused by PE-MPs, monocyte chemoattractant protein-1 and tumor necrosis factor-alpha were increased compared to the control group except for intratracheal intilation-high concentration PE-MPs. The C-reactive protein level was decreased by intragastric administration compared to the control group and intratracheal instillation was increased compared to the control group. Conclusions: Despite the difficulty in comparing the toxic intensity between intragastric administration and intratracheal instillation of PE-MPs, our study revealed that oxidative stress and inflammation were induced in the neonatal liver. However, it is necessary to evaluate the toxic effects of microplastics on various organs as well. Overall, the present study indicates that the evaluation of toxic effects of long-term microplastic exposure, potential of microplastic toxicity on next-generation offspring and toxicity mechanism in human should be considered for further investigations.
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妊娠小鼠胃内或气管内灌注聚乙烯微塑料对新生儿肝脏毒性的评价
摘要背景:目前的研究表明,人类通过食用食品和饮料、通过气道和各种其他途径暴露于微塑料。目的:我们通过给药或气管内给药的方式评估聚乙烯微塑料(PE-MPs)在妊娠小鼠新生儿肝脏中的氧化应激和炎症。方法:从妊娠第9天至出生后第7天给予PE-MPs。PE-MPs分为灌胃组(0.01 mg/小鼠/天或0.1 mg/小鼠/天)和气管内滴注组(6 μ g/小鼠/天或60 μ g/小鼠/天)。牺牲后,测定新生儿肝脏氧化应激和炎症反应。结果:由于PE-MPs在新生儿肝脏中引起氧化应激,与对照组相比,灌胃组谷胱甘肽过氧化物酶呈浓度依赖性下降,高浓度PE-MPs气管内滴注降低。高浓度灌胃和气管内灌注时过氧化氢酶水平升高。为了证实PE-MPs引起的炎症水平,除了气管内膨胀-高浓度PE-MPs外,单核细胞趋化蛋白-1和肿瘤坏死因子- α均比对照组升高。与对照组相比,灌胃组c反应蛋白水平降低,气管内滴注组c反应蛋白水平升高。结论:尽管PE-MPs灌胃和气管内滴注的毒性强度难以比较,但我们的研究表明,PE-MPs在新生儿肝脏中诱导了氧化应激和炎症。然而,也有必要评估微塑料对各器官的毒性作用。综上所述,本研究表明,微塑料长期暴露的毒性效应评估、微塑料对下一代的潜在毒性以及对人体的毒性机制有待进一步研究。
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