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下一代测序揭示了人肺细胞对急性与长期暴露于氧化石墨烯的不同反应。

Next-Generation Sequencing Reveals Differential Responses to Acute versus Long-Term Exposures to Graphene Oxide in Human Lung Cells.

作者信息

Mukherjee Sourav P, Gupta Govind, Klöditz Katharina, Wang Jun, Rodrigues Artur Filipe, Kostarelos Kostas, Fadeel Bengt

机构信息

Nanosafety and Nanomedicine Laboratory, Division of Molecular Toxicology, Institute of Environmental Medicine, Karolinska Institutet, Stockholm, 171 77, Sweden.

Science for Life Laboratory, Department of Biochemistry and Biophysics, Stockholm University, Stockholm, 106 91, Sweden.

出版信息

Small. 2020 May;16(21):e1907686. doi: 10.1002/smll.201907686. Epub 2020 Mar 29.

Abstract

Numerous studies have addressed the biological impact of graphene-based materials including graphene oxide (GO), yet few have focused on long-term effects. Here, RNA sequencing is utilized to unearth responses of human lung cells to GO. To this end, the BEAS-2B cell line derived from normal human bronchial epithelium is subjected to repeated, low-dose exposures of GO (1 or 5 µg mL ) for 28 days or to the equivalent, cumulative amount of GO for 48 h. Then, samples are analyzed by using the NovaSeq 6000 sequencing system followed by pathway analysis and gene ontology enrichment analysis of the differentially expressed genes. Significant differences are seen between the low-dose, long-term exposures and the high-dose, short-term exposures. Hence, exposure to GO for 48 h results in mitochondrial dysfunction. In contrast, exposure to GO for 28 days is characterized by engagement of apoptosis pathways with downregulation of genes belonging to the inhibitor of apoptosis protein (IAP) family. Validation experiments confirm that long-term exposure to GO affects the apoptosis threshold in lung cells, accompanied by a loss of IAPs. These studies reveal the sensitivity of RNA-sequencing approaches and show that acute exposure to GO is not a good predictor of the long-term effects of GO.

摘要

许多研究都探讨了包括氧化石墨烯(GO)在内的基于石墨烯材料的生物学影响,但很少有研究关注其长期影响。在此,利用RNA测序来揭示人肺细胞对GO的反应。为此,将源自正常人支气管上皮的BEAS-2B细胞系反复低剂量暴露于GO(1或5μg/mL)28天,或暴露于等量累积量的GO 48小时。然后,使用NovaSeq 6000测序系统对样本进行分析,随后对差异表达基因进行通路分析和基因本体富集分析。低剂量长期暴露和高剂量短期暴露之间存在显著差异。因此,暴露于GO 48小时会导致线粒体功能障碍。相比之下,暴露于GO 28天的特征是凋亡途径的激活以及凋亡抑制蛋白(IAP)家族基因的下调。验证实验证实,长期暴露于GO会影响肺细胞的凋亡阈值,并伴有IAPs的丧失。这些研究揭示了RNA测序方法的敏感性,并表明急性暴露于GO并不能很好地预测GO的长期影响。

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