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在生理氧水平下培养癌细胞以细胞类型特异性方式影响基因表达。

Culture of Cancer Cells at Physiological Oxygen Levels Affects Gene Expression in a Cell-Type Specific Manner.

机构信息

Department of Biological Sciences, Brock University, St. Catharines, ON L2S 3A1, Canada.

Centre for Biotechnology, Brock University, St. Catharines, ON L2S 3A1, Canada.

出版信息

Biomolecules. 2022 Nov 14;12(11):1684. doi: 10.3390/biom12111684.

Abstract

Standard cell culture is routinely performed at supraphysiological oxygen levels (~18% O). Conversely, O levels in most mammalian tissues range from 1-6% (physioxia). Such hyperoxic conditions in cell culture can alter reactive oxygen species (ROS) production, metabolism, mitochondrial networks, and response to drugs and hormones. The aim of this study was to investigate the transcriptional response to different O levels and determine whether it is similar across cell lines, or cell line-specific. Using RNA-seq, we performed differential gene expression and functional enrichment analyses in four human cancer cell lines, LNCaP, Huh-7, PC-3, and SH-SY5Y cultured at either 5% or 18% O for 14 days. We found that O levels affected transcript abundance of thousands of genes, with the affected genes having little overlap between cell lines. Functional enrichment analysis also revealed different processes and pathways being affected by O in each cell line. Interestingly, most of the top differentially expressed genes are involved in cancer biology, which highlights the importance of O levels in cancer cell research. Further, we observed several hypoxia-inducible factor (HIF) targets, HIF-2α targets particularly, upregulated at 5% O, consistent with a role for HIFs in physioxia. O levels also differentially induced the transcription of mitochondria-encoded genes in most cell lines. Finally, by comparing our transcriptomic data from LNCaP and PC-3 with datasets from the Prostate Cancer Transcriptome Atlas, a correlation between genes upregulated at 5% O in LNCaP cells and the in vivo prostate cancer transcriptome was found. We conclude that the transcriptional response to O over the range from 5-18% is robust and highly cell-type specific. This latter finding indicates that the effects of O levels are difficult to predict and thus highlights the importance of regulating O in cell culture.

摘要

常规的细胞培养是在超生理氧水平(~18% O)下进行的。相反,大多数哺乳动物组织中的 O 水平范围为 1-6%(低氧)。细胞培养中的这种高氧条件会改变活性氧(ROS)的产生、代谢、线粒体网络以及对药物和激素的反应。本研究旨在研究不同 O 水平下的转录反应,并确定其是否在细胞系之间相似,或者是细胞系特异性的。使用 RNA-seq,我们在四种人类癌细胞系(LNCaP、Huh-7、PC-3 和 SH-SY5Y)中进行了差异基因表达和功能富集分析,这些细胞系分别在 5%或 18% O 下培养 14 天。我们发现 O 水平影响了数千个基因的转录丰度,而受影响的基因在细胞系之间几乎没有重叠。功能富集分析还揭示了 O 对每个细胞系中不同过程和途径的影响。有趣的是,大多数差异表达基因都与癌症生物学有关,这凸显了 O 水平在癌症细胞研究中的重要性。此外,我们观察到几个缺氧诱导因子(HIF)靶标,特别是 HIF-2α 靶标,在 5% O 下上调,这与 HIFs 在低氧中的作用一致。O 水平还在大多数细胞系中差异诱导了线粒体编码基因的转录。最后,通过将我们从 LNCaP 和 PC-3 获得的转录组数据与前列腺癌转录组图谱中的数据集进行比较,发现 LNCaP 细胞中 5% O 上调的基因与体内前列腺癌转录组之间存在相关性。我们得出结论,O 水平在 5-18%范围内的转录反应是稳健的,并且高度细胞类型特异性。后一种发现表明 O 水平的影响难以预测,因此凸显了在细胞培养中调节 O 的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b01/9688152/f31185d4458e/biomolecules-12-01684-g001.jpg

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