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通过RNA测序检测到的原代人成纤维细胞中保守的衰老相关基因和通路

Conserved Senescence Associated Genes and Pathways in Primary Human Fibroblasts Detected by RNA-Seq.

作者信息

Marthandan S, Baumgart M, Priebe S, Groth M, Schaer J, Kaether C, Guthke R, Cellerino A, Platzer M, Diekmann S, Hemmerich P

机构信息

Leibniz-Institute on Aging-Fritz Lipmann Institute e.V. (FLI), Jena, Germany.

Leibniz Institute for Natural Product Research and Infection Biology-Hans-Knöll-Institute e.V. (HKI), Jena, Germany.

出版信息

PLoS One. 2016 May 3;11(5):e0154531. doi: 10.1371/journal.pone.0154531. eCollection 2016.

Abstract

Cellular senescence correlates with changes in the transcriptome. To obtain a complete view on senescence-associated transcription networks and pathways, we assessed by deep RNA sequencing the transcriptomes of five of the most commonly used laboratory strains of human fibroblasts during their transition into senescence. In a number of cases, we verified the RNA-seq data by real-time PCR. By determining cellular protein levels we observed that the age-related expression of most but not all genes is regulated at the transcriptional level. We found that 78% of the age-affected differentially expressed genes were commonly regulated in the same direction (either up- or down-regulated) in all five fibroblast strains, indicating a strong conservation of age-associated changes in the transcriptome. KEGG pathway analyses confirmed up-regulation of the senescence-associated secretory phenotype and down-regulation of DNA synthesis/repair and most cell cycle pathways common in all five cell strains. Newly identified senescence-induced pathways include up-regulation of endocytotic/phagocytic pathways and down-regulation of the mRNA metabolism and the mRNA splicing pathways. Our results provide an unprecedented comprehensive and deep view into the individual and common transcriptome and pathway changes during the transition into of senescence of five human fibroblast cell strains.

摘要

细胞衰老与转录组变化相关。为全面了解衰老相关的转录网络和途径,我们通过深度RNA测序评估了五种最常用的人类成纤维细胞实验室菌株在进入衰老过程中的转录组。在许多情况下,我们通过实时PCR验证了RNA测序数据。通过测定细胞蛋白水平,我们观察到大多数但并非所有基因的年龄相关表达在转录水平上受到调控。我们发现,在所有五种成纤维细胞菌株中,78%受年龄影响的差异表达基因通常在相同方向(上调或下调)受到调控,这表明转录组中与年龄相关的变化具有很强的保守性。KEGG通路分析证实,衰老相关分泌表型上调,DNA合成/修复以及所有五种细胞菌株共有的大多数细胞周期通路下调。新发现的衰老诱导通路包括内吞/吞噬通路上调以及mRNA代谢和mRNA剪接通路下调。我们的结果为五种人类成纤维细胞菌株进入衰老过程中个体和共同的转录组及通路变化提供了前所未有的全面而深入的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/61df/4854426/8ba810f0586a/pone.0154531.g001.jpg

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