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首页> 外文期刊>Journal of molecular cell biology >A combined computational pipeline to detect circular RNAs in human cancer cells under hypoxic stress
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A combined computational pipeline to detect circular RNAs in human cancer cells under hypoxic stress

机译:在缺氧应力下检测人癌细胞中圆形RNA的组合计算管道

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摘要

Hypoxia is associated with several diseases, including cancer. Cells that are deprived of adequate oxygen supply trigger tran-scriptional and post-transcriptional responses, which control cellular pathways such as angiogenesis, proliferation, and metabolic adaptation. Circular RNAs (circRNAs) are a novel class of mainly non-coding RNAs, which have been implicated in multiple cancers and attract increasing attention as potential biomarkers. Here, we characterize the circRNA signatures of three different cancer cell lines from cervical (HeLa), breast (MCF-7), and lung (A549) cancer under hypoxia. In order to reliably detect circRNAs, we integrate available tools with custom approaches for quantification and statistical analysis. Using this consolidated computational pipeline, we identify approx12000 circRNAs in the three cancer cell lines. Their molecular characteristics point to an involvement of complementary RNA sequences as well as trans-acting factors in circRNA biogenesis, such as the RNA-binding protein HNRNPC. Notably, we detect a number of circRNAs that are more abundant than their linear counterparts. In addition, 64 circRNAs significantly change in abundance upon hypoxia, in most cases in a cell type-specific manner. In summary, we present a comparative circRNA profiling in human cancer cell lines, which promises novel insights into the biogenesis and function of circRNAs under hypoxic stress.
机译:缺氧与几种疾病有关,包括癌症。被剥夺了足够的氧气供应触发的细胞触发器触发术和转录后反应,其控制细胞途径,例如血管生成,增殖和代谢适应。圆形RNA(CircRNA)是一种主要的主要非编码RNA类,其涉及多种癌症并吸引越来越受到潜在的生物标志物。在这里,我们在缺氧下的宫颈(HELA),乳腺(MCF-7)和肺(A549)癌症中三种不同癌细胞系的Circrna签名。为了可靠地检测CircRNA,我们将可用的工具集成了定制方法,以进行量化和统计分析。使用这种综合的计算管道,我们在三种癌细胞系中识别大约12000个CircrNA。它们的分子特性指向互补RNA序列的累及以及CircrNA生物发生中的反式作用因子,例如RNA结合蛋白HNRNPC。值得注意的是,我们发现了许多比其线性对应物更丰富的Circrnas。此外,在细胞类型特异性的大多数情况下,64个Circrnas在缺氧时大量变化。总之,我们在人类癌细胞系中提出了一种比较圆形谱分析,这对缺氧应力下的核心生物发生和功能的生物发生和功能有望。

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