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一种用于在呼吸式肺芯片系统上研究肺损伤和毒性的新型永生化人肺泡上皮细胞模型。

A New Immortalized Human Alveolar Epithelial Cell Model to Study Lung Injury and Toxicity on a Breathing Lung-On-Chip System.

作者信息

Sengupta Arunima, Roldan Nuria, Kiener Mirjam, Froment Laurène, Raggi Giulia, Imler Theo, de Maddalena Lea, Rapet Aude, May Tobias, Carius Patrick, Schneider-Daum Nicole, Lehr Claus-Michael, Kruithof-de Julio Marianna, Geiser Thomas, Marti Thomas Michael, Stucki Janick D, Hobi Nina, Guenat Olivier T

机构信息

Organs-on-Chip Technologies, ARTORG Center for Biomedical Engineering, University of Bern, Bern, Switzerland.

Alveolix AG, Swiss Organs-on-Chip Innovation, Bern, Switzerland.

出版信息

Front Toxicol. 2022 Jun 17;4:840606. doi: 10.3389/ftox.2022.840606. eCollection 2022.

Abstract

The evaluation of inhalation toxicity, drug safety and efficacy assessment, as well as the investigation of complex disease pathomechanisms, are increasingly relying on lung models. This is due to the progressive shift towards human-based systems for more predictive and translational research. While several cellular models are currently available for the upper airways, modelling the distal alveolar region poses several constraints that make the standardization of reliable alveolar models relatively difficult. In this work, we present a new and reproducible alveolar model, that combines a human derived immortalized alveolar epithelial cell line (iAEC) and organ-on-chip technology mimicking the lung alveolar biophysical environment (lung-on-chip). The latter mimics key features of the alveolar milieu: breathing-like 3D cyclic stretch (10% linear strain, 0.2 Hz frequency) and an ultrathin, porous and elastic membrane. iAECs cultured on-chip were characterized for their alveolar epithelial cell markers by gene and protein expression. Cell barrier properties were examined by TER (Transbarrier Electrical Resistance) measurement and tight junction formation. To establish a physiological model for the distal lung, iAECs were cultured for long-term at air-liquid interface (ALI) on-chip. To this end, different stages of alveolar damage including inflammation (via exposure to bacterial lipopolysaccharide) and the response to a profibrotic mediator (via exposure to Transforming growth factor β1) were analyzed. In addition, the expression of relevant host cell factors involved in SARS-CoV-2 infection was investigated to evaluate its potential application for COVID-19 studies. This study shows that iAECs cultured on the lung-on-chip exhibit an enhanced in vivo-like alveolar character which is reflected into: 1) Alveolar type 1 (AT1) and 2 (AT2) cell specific phenotypes, 2) tight barrier formation (with TER above 1,000 Ω cm) and 3) reproducible long-term preservation of alveolar characteristics in nearly physiological conditions (co-culture, breathing, ALI). To the best of our knowledge, this is the first time that a primary derived alveolar epithelial cell line on-chip representing both AT1 and AT2 characteristics is reported. This distal lung model thereby represents a valuable tool to study inhalation toxicity, test safety and efficacy of drug compounds and characterization of xenobiotics.

摘要

吸入毒性评估、药物安全性和有效性评估以及复杂疾病发病机制的研究越来越依赖于肺模型。这是因为研究正逐渐向基于人体的系统转变,以进行更具预测性和转化性的研究。虽然目前有几种用于上呼吸道的细胞模型,但对远端肺泡区域进行建模存在一些限制,这使得可靠的肺泡模型标准化相对困难。在这项工作中,我们提出了一种新的、可重复的肺泡模型,它结合了源自人类的永生化肺泡上皮细胞系(iAEC)和模拟肺泡生物物理环境的芯片器官技术(肺芯片)。后者模拟了肺泡环境的关键特征:类似呼吸的3D周期性拉伸(10%线性应变,0.2Hz频率)以及超薄、多孔且有弹性的膜。在芯片上培养的iAEC通过基因和蛋白质表达对其肺泡上皮细胞标志物进行了表征。通过跨膜电阻(TER)测量和紧密连接形成来检查细胞屏障特性。为了建立远端肺的生理模型,iAEC在芯片上的气液界面(ALI)进行长期培养。为此,分析了肺泡损伤的不同阶段,包括炎症(通过暴露于细菌脂多糖)和对促纤维化介质的反应(通过暴露于转化生长因子β1)。此外,还研究了参与SARS-CoV-2感染的相关宿主细胞因子的表达,以评估其在COVID-19研究中的潜在应用。这项研究表明,在肺芯片上培养的iAEC表现出增强的类似体内的肺泡特征,这体现在:1)1型肺泡(AT1)和2型肺泡(AT2)细胞的特异性表型;2)紧密屏障形成(TER高于1000Ω·cm);3)在近乎生理条件下(共培养、呼吸、ALI)可重复长期保持肺泡特征。据我们所知,这是首次报道一种代表AT1和AT2特征的芯片上原代衍生肺泡上皮细胞系。因此,这种远端肺模型是研究吸入毒性、测试药物化合物安全性和有效性以及表征异生物素的有价值工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a17/9272139/de0d43516424/ftox-04-840606-g001.jpg

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