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首页> 外文期刊>International journal of computational biology and drug design >Evaluation of biological and technical variations in low-input RNA-Seq and single-cell RNA-Seq
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Evaluation of biological and technical variations in low-input RNA-Seq and single-cell RNA-Seq

机译:低输入RNA-SEQ和单细胞RNA-SEQ的生物和技术变异评估

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Background: Low-input or single-cell RNA-Seq are widely used today, but two technical questions remain: 1) in technical replicates, what proportion of noises comes from input RNA quantity rather than variation of bioinformatics tools?; 2) In single neurons, whether variation in gene expression is attributable to biological heterogeneity or just random noise? To examine the sources of variability, we have generated RNA-Seq data from low-input (10/100/1000pg) reference RNA samples and 38 single neurons from human brains. Results: For technical replicates, the quantity of input RNA is negatively correlated with expression variation. For genes in the medium- and high-expression groups, input RNA amount explains most of the variation, whereas bioinformatic pipelines explain some variation for the low-expression group. The t-distributed stochastic neighbour embedding (t-SNE) method reveals data-inherent aggregation of low-input replicate data, and suggests heterogeneity of single pyramidal neuron transcriptome. Interestingly, expression variation in single neurons is biologically relevant. Conclusions: We found that differences in bioinformatics pipelines do not present a major source of variation.
机译:背景:低输入或单细胞RNA-SEQ今天广泛使用,但仍然存在两个技术问题:1)在技术复制中,噪声比例来自输入RNA量而不是生物信息学工具的变异? 2)在单一神经元中,基因表达的变异是否可归因于生物异质性或只是随机噪声?为了检查可变性来源,我们从低输入(10/100/10000 / 10000pg)参考RNA样品和来自人脑的38个单一神经元产生了RNA-SEQ数据。结果:对于技术复制,输入RNA的量与表达变化负相关。对于中等和高表达组中的基因,输入RNA量解释了大部分变化,而生物信息管道解释了低表达组的一些变化。 T分布式随机邻居嵌入(T-SNE)方法揭示了低输入重复数据的数据固有聚集,并表明单个金字塔神经元转录组的异质性。有趣的是,单一神经元的表达变异是生物学相关的。结论:我们发现生物信息化管道的差异不会出现主要的变异来源。

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