Stress granule formation as a marker of cellular toxicity in lung organoids

Seung-Yeon Kim, Kee K. Kim, Eun-Mi Kim
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Abstract

Cells regulate protein synthesis under stressful circumstances by forming cytoplasmic RNA granules, termed stress granules (SGs). SGs are membrane-less organelles that function as a protective mechanism in response to stress. They function through liquid-liquid phase separation, which is a vital process comprising 2 distinct de-mixed liquid phases. The components of SGs, such as G3BP1, can serve as biomarkers of cell toxicity. Respiratory diseases are among the leading causes of death globally. After the humidifier disinfectant disaster in Korea in 2011, social concerns over respiratory disease-related deaths have been raised, and the importance of inhalation toxicity testing has been emphasized. Traditionally, in vivo animal models have been used to assess inhalation toxicity, but these models still have limitations owing to physiological differences between species. To overcome these limitations, human immortalized lung epithelial and lung cancer cell lines have been used to evaluate lung toxicity in vitro. Human stem cell-derived 3-dimensional organoid technology has recently been developed in various research fields, including lung toxicity. This review discusses SG-related proteins as potential biomarkers for lung toxicity assessment, especially in human lung organoids under stress conditions, such as exposure to toxic chemicals.
应激颗粒形成作为肺类器官细胞毒性的标志
在应激环境下,细胞通过形成胞质RNA颗粒(称为应激颗粒)来调节蛋白质合成。SGs是一种无膜细胞器,可作为应激反应的保护机制。它们通过液-液相分离发挥作用,这是一个由两个不同的脱混液相组成的重要过程。SGs的组分,如G3BP1,可以作为细胞毒性的生物标志物。呼吸系统疾病是全球主要死亡原因之一。2011年韩国发生“加湿器消毒液灾难”后,呼吸系统疾病相关死亡的社会担忧不断增加,吸入毒性检测的重要性日益受到重视。传统上,体内动物模型已被用于评估吸入毒性,但由于物种之间的生理差异,这些模型仍然存在局限性。为了克服这些局限性,人类永生化肺上皮细胞和肺癌细胞系被用于体外评估肺毒性。人类干细胞衍生的三维类器官技术最近在包括肺毒性在内的各个研究领域得到了发展。这篇综述讨论了sg相关蛋白作为肺毒性评估的潜在生物标志物,特别是在应激条件下,如暴露于有毒化学物质的人类肺类器官。
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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