Transferability and reproducibility of exposed air-liquid interface co-culture lung models

IF 4.7 3区 环境科学与生态学 Q2 ENVIRONMENTAL SCIENCES NanoImpact Pub Date : 2023-07-01 DOI:10.1016/j.impact.2023.100466
Hedwig M. Braakhuis , Eric R. Gremmer , Anne Bannuscher , Barbara Drasler , Sandeep Keshavan , Barbara Rothen-Rutishauser , Barbara Birk , Andreas Verlohner , Robert Landsiedel , Kirsty Meldrum , Shareen H. Doak , Martin J.D. Clift , Johanna Samulin Erdem , Oda A.H. Foss , Shanbeh Zienolddiny-Narui , Tommaso Serchi , Elisa Moschini , Pamina Weber , Sabina Burla , Pramod Kumar , Rob J. Vandebriel
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引用次数: 3

Abstract

Background

The establishment of reliable and robust in vitro models for hazard assessment, a prerequisite for moving away from animal testing, requires the evaluation of model transferability and reproducibility. Lung models that can be exposed via the air, by means of an air-liquid interface (ALI) are promising in vitro models for evaluating the safety of nanomaterials (NMs) after inhalation exposure. We performed an inter-laboratory comparison study to evaluate the transferability and reproducibility of a lung model consisting of the human bronchial cell line Calu-3 as a monoculture and, to increase the physiologic relevance of the model, also as a co-culture with macrophages (either derived from the THP-1 monocyte cell line or from human blood monocytes). The lung model was exposed to NMs using the VITROCELL® Cloud12 system at physiologically relevant dose levels.

Results

Overall, the results of the 7 participating laboratories are quite similar. After exposing Calu-3 alone and Calu-3 co-cultures with macrophages, no effects of lipopolysaccharide (LPS), quartz (DQ12) or titanium dioxide (TiO2) NM-105 particles on the cell viability and barrier integrity were detected. LPS exposure induced moderate cytokine release in the Calu-3 monoculture, albeit not statistically significant in most labs. In the co-culture models, most laboratories showed that LPS can significantly induce cytokine release (IL-6, IL-8 and TNF-α). The exposure to quartz and TiO2 particles did not induce a statistically significant increase in cytokine release in both cell models probably due to our relatively low deposited doses, which were inspired by in vivo dose levels. The intra- and inter-laboratory comparison study indicated acceptable interlaboratory variation for cell viability/toxicity (WST-1, LDH) and transepithelial electrical resistance, and relatively high inter-laboratory variation for cytokine production.

Conclusion

The transferability and reproducibility of a lung co-culture model and its exposure to aerosolized particles at the ALI were evaluated and recommendations were provided for performing inter-laboratory comparison studies. Although the results are promising, optimizations of the lung model (including more sensitive read-outs) and/or selection of higher deposited doses are needed to enhance its predictive value before it may be taken further towards a possible OECD guideline.

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暴露空气-液体界面共培养肺模型的可转移性和再现性。
背景:建立可靠和稳健的体外危险评估模型是放弃动物试验的先决条件,需要评估模型的可转移性和再现性。可以通过空气-液体界面(ALI)通过空气暴露的肺部模型是评估吸入暴露后纳米材料(NMs)安全性的有前景的体外模型。我们进行了一项实验室间比较研究,以评估由人类支气管细胞系Calu-3组成的肺模型的可转移性和再现性,该模型作为单一培养物,并且为了增加该模型的生理相关性,也作为与巨噬细胞(来源于THP-1单核细胞系或来源于人类血液单核细胞)的共培养物。使用VITROCELL®Cloud12系统将肺模型暴露于生理相关剂量水平的NMs。结果:总体而言,7个参与实验室的结果非常相似。单独暴露Calu-3和Calu-3与巨噬细胞共培养后,未检测到脂多糖(LPS)、石英(DQ12)或二氧化钛(TiO2)NM-105颗粒对细胞活力和屏障完整性的影响。LPS暴露在Calu-3单一培养中诱导了适度的细胞因子释放,尽管在大多数实验室中没有统计学意义。在共培养模型中,大多数实验室表明LPS可以显著诱导细胞因子(IL-6、IL-8和TNF-α)的释放。暴露于石英和TiO2颗粒并没有在两种细胞模型中诱导细胞因子释放的统计学显著增加,这可能是由于我们的沉积剂量相对较低,这是受体内剂量水平的启发。实验室内和实验室间比较研究表明,细胞活力/毒性(WST-1、LDH)和跨上皮电阻的实验室间变化是可接受的,细胞因子产生的实验室间差异相对较高。结论:评估了肺共培养模型的可转移性和再现性,并为进行实验室间比较研究提供了建议。尽管结果很有希望,但在进一步制定可能的经合组织指南之前,需要优化肺部模型(包括更敏感的读数)和/或选择更高的沉积剂量,以提高其预测价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
NanoImpact
NanoImpact Social Sciences-Safety Research
CiteScore
11.00
自引率
6.10%
发文量
69
审稿时长
23 days
期刊介绍: NanoImpact is a multidisciplinary journal that focuses on nanosafety research and areas related to the impacts of manufactured nanomaterials on human and environmental systems and the behavior of nanomaterials in these systems.
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