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ShrinkBayes: a versatile R-package for analysis of count-based sequencing data in complex study designs

机译:ShrinkBayes:多功能R包,用于分析复杂研究设计中基于计数的测序数据

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摘要

Background: Complex designs are common in (observational) clinical studies. Sequencing data for such studies are produced more and more often, implying challenges for the analysis, such as excess of zeros, presence of random effects and multi-parameter inference. Moreover, when sample sizes are small, inference is likely to be too liberal when, in a Bayesian setting, applying a non-appropriate prior or to lack power when not carefully borrowing information across features.Results: We show on microRNA sequencing data from a clinical cancer study how our software ShrinkBayes tackles the aforementioned challenges. In addition, we illustrate its comparatively good performance on multi-parameter inference for groups using a data-based simulation. Finally, in the small sample size setting, we demonstrate its high power and improved FDR estimation by use of Gaussian mixture priors that include a point mass.Conclusion: ShrinkBayes is a versatile software package for the analysis of count-based sequencing data, which is particularly useful for studies with small sample sizes or complex designs. © 2014 van de Wiel et al.; licensee BioMed Central Ltd.
机译:背景:复杂的设计在(观察)临床研究中很常见。用于此类研究的测序数据越来越频繁,这暗示了分析的挑战,例如过多的零,存在随机效应和多参数推断。此外,当样本量较小时,在贝叶斯环境中应用不适当的先验或在不仔细借用跨特征信息的情况下缺乏能力的情况下,推断可能过于宽松。临床癌症研究我们的软件ShrinkBayes如何解决上述挑战。此外,我们使用基于数据的仿真说明了其在多参数推理组中的相对较好的性能。最后,在小样本量的环境中,我们通过使用包括点质量的高斯混合先验证明了其强大的功能和改进的FDR估计。结论:ShrinkBayes是一款多功能软件包,可用于分析基于计数的测序数据,即对于小样本量或复杂设计的研究特别有用。 ©2014 van de Wiel等;被许可人BioMed Central Ltd.

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