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开发一种接触点吸入毒性测试挥发性化合物的体外方法,使用器官型培养和气液界面暴露。

Development of an in vitro approach to point-of-contact inhalation toxicity testing of volatile compounds, using organotypic culture and air-liquid interface exposure.

机构信息

ScitoVation, LLC, Durham, NC 27713, United States.

ScitoVation, LLC, Durham, NC 27713, United States.

出版信息

Toxicol In Vitro. 2020 Dec;69:104968. doi: 10.1016/j.tiv.2020.104968. Epub 2020 Aug 15.

Abstract

In vitro chemical risk assessment using human cells is emerging as an alternative to in vivo animal testing with reduced costs, fewer animal welfare concerns, and the possibility of greater human health relevance. In vitro inhalation toxicity testing of volatile compounds poses particular challenges. Here we report our efforts to establish a testing protocol in our own lab using the EpiAirway bronchial epithelium cell culture model and the Vitrocell 12/12 system for air-liquid interface (ALI) exposures. For purposes of method development, we used methyl iodide (MeI) as a test compound. We examined viability, cytotoxicity, and epithelial integrity responses. Dose-dependent, reproducible responses were observed with all assays. EpiAirway and BEAS-2B cytotoxicity responses to acute exposure were roughly similar, but EpiAirway was more resistant than BEAS-2B by the viability measurement, suggesting a proliferative response at low MeI concentrations. If wells were sealed to prevent evaporation, in-solution MeI concentration-response could be used to predict the response to MeI vapor within 2-fold by converting from the media- to the air-concentration at equilibrium using the blood:air partition coefficient for MeI. The long-term stability of EpiAirway cultures enabled repeated exposures over a 5-d period, which produced responses at lower concentrations than did acute exposure.

摘要

利用人体细胞进行体外化学风险评估正在兴起,作为替代体内动物测试的方法,这种方法具有降低成本、减少动物福利问题的关注以及更大的人类健康相关性的可能性。挥发性化合物的体外吸入毒性测试带来了特殊的挑战。在这里,我们报告了我们在自己的实验室中使用 EpiAirway 支气管上皮细胞培养模型和 Vitrocell 12/12 系统进行空气-液体界面 (ALI) 暴露来建立测试方案的努力。出于方法开发的目的,我们使用碘化甲基 (MeI) 作为测试化合物。我们检查了细胞活力、细胞毒性和上皮完整性反应。所有测定均观察到剂量依赖性、可重现的反应。EpiAirway 和 BEAS-2B 对急性暴露的细胞毒性反应大致相似,但通过活力测量,EpiAirway 比 BEAS-2B 更具抗性,这表明在低 MeI 浓度下存在增殖反应。如果将孔密封以防止蒸发,则可以使用溶液中的 MeI 浓度-反应来预测通过从平衡时的介质浓度转换为空气浓度来预测 MeI 蒸气的反应,使用 MeI 的血液:空气分配系数。EpiAirway 培养物的长期稳定性使得可以在 5 天的时间内进行重复暴露,从而在较低浓度下产生反应,而急性暴露则不会产生反应。

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