Fifteen day repeat air: liquid Interface air-only exposures can cause respiratory epithelium injury in MucilAir nasal respiratory epithelial cells that parallels chemically induced cytotoxicity.

IF 3.2 4区 医学 Q1 Pharmacology, Toxicology and Pharmaceutics Toxicology Mechanisms and Methods Pub Date : 2024-07-30 DOI:10.1080/15376516.2024.2382794
Leslie Recio, Raymond Samuel, Susan A Elmore, Jamie Scaglione
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Abstract

New Approach Methodologies (NAMs) are being widely used to reduce, refine, and replace, animal use in studying toxicology. For respiratory toxicology, this includes in silico and in vitro alternatives using air:liquid interface (ALI) exposures to replace traditional in vivo inhalation studies. In previous studies using 1,3-dichloropropene (1,3-DCP), a 5-day 4 h repeat exposures of MucilAir nasal cell culture models caused, dose-dependent cytotoxicity, depletion of GSH, changes in differential gene expression and histopathological transitions in cellular morphology from pseudostratified columnar epithelium to squamous epithelium. In this report we attempted to extend these studies using 15-day 1,3-DCP 4 h exposures to using MucilAir nasal cultures as outlined by an US EPA recent task order (US EPA 2023). For the 15-day repeat exposure, there were severe histopathologic changes in the MucilAir nasal mock-treatment (air-only) VITROCELL® chamber controls compared to incubator controls preventing any further analysis. The histopathological transitions in cellular morphology from pseudostratified columnar epithelium to squamous epithelium observed in the air only control in this study and previously with 1,3-DCP in MucilAir nasal cultures is also a hallmark of chemically induced cytotoxic responses in vivo in the respiratory tract. Histopathology assessments of 3D respiratory tract models used in ALI exposures can provide the linkage between in vitro to in vivo outcomes as part of the validation efforts of ALI use in regulatory toxicology. This report indicates that importance of histopathological assessments of incubator and mock-treatment (air-only) controls from each ALI exposure experiment along with exposed cell based model.

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在 MucilAir™ 鼻呼吸道上皮细胞中,15 天重复接触空气:仅接触液体界面空气会造成呼吸道上皮细胞损伤,这种损伤与化学诱导的细胞毒性相似。
新方法(NAMs)正被广泛用于减少、改进和替代毒理学研究中的动物实验。在呼吸毒理学方面,这包括使用空气:液体界面(ALI)暴露的硅学和体外替代方法,以取代传统的体内吸入研究。在之前使用 1,3-二氯丙烯(1,3-DCP)进行的研究中,对 MucilAir™ 鼻细胞培养模型进行 5 天 4 小时的重复暴露会导致剂量依赖性细胞毒性、GSH 消耗、不同基因表达的变化以及细胞形态从假柱状上皮到鳞状上皮的组织病理学转变。在本报告中,我们尝试按照美国环保局最近下达的任务指令(US EPA 2023),使用 MucilAir™ 鼻腔培养物进行为期 15 天的 1,3-DCP 4 小时暴露,从而扩展这些研究。在为期 15 天的重复暴露中,MucilAir™ 鼻腔模拟处理(纯空气)VITROCELL® 室对照组与培养箱对照组相比出现了严重的组织病理学变化,因此无法进行进一步分析。在本研究中的纯空气对照组和之前在 MucilAir™ 鼻腔培养物中使用 1,3-DCP 时观察到的细胞形态从假柱状上皮到鳞状上皮的组织病理学转变,也是呼吸道中化学诱导的体内细胞毒性反应的标志。对 ALI 暴露中使用的三维呼吸道模型进行组织病理学评估,可将体外结果与体内结果联系起来,作为 ALI 用于监管毒理学验证工作的一部分。本报告指出了对每次 ALI 暴露实验中的培养箱和模拟处理(纯空气)对照组以及基于暴露细胞的模型进行组织病理学评估的重要性。
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来源期刊
CiteScore
6.60
自引率
3.10%
发文量
66
审稿时长
6-12 weeks
期刊介绍: Toxicology Mechanisms and Methods is a peer-reviewed journal whose aim is twofold. Firstly, the journal contains original research on subjects dealing with the mechanisms by which foreign chemicals cause toxic tissue injury. Chemical substances of interest include industrial compounds, environmental pollutants, hazardous wastes, drugs, pesticides, and chemical warfare agents. The scope of the journal spans from molecular and cellular mechanisms of action to the consideration of mechanistic evidence in establishing regulatory policy. Secondly, the journal addresses aspects of the development, validation, and application of new and existing laboratory methods, techniques, and equipment. A variety of research methods are discussed, including: In vivo studies with standard and alternative species In vitro studies and alternative methodologies Molecular, biochemical, and cellular techniques Pharmacokinetics and pharmacodynamics Mathematical modeling and computer programs Forensic analyses Risk assessment Data collection and analysis.
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