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通过替代变量分析在基因表达研究中捕捉异质性。

Capturing heterogeneity in gene expression studies by surrogate variable analysis.

作者信息

Leek Jeffrey T, Storey John D

机构信息

Department of Biostatistics, University of Washington, Seattle, Washington, USA.

出版信息

PLoS Genet. 2007 Sep;3(9):1724-35. doi: 10.1371/journal.pgen.0030161. Epub 2007 Aug 1.

Abstract

It has unambiguously been shown that genetic, environmental, demographic, and technical factors may have substantial effects on gene expression levels. In addition to the measured variable(s) of interest, there will tend to be sources of signal due to factors that are unknown, unmeasured, or too complicated to capture through simple models. We show that failing to incorporate these sources of heterogeneity into an analysis can have widespread and detrimental effects on the study. Not only can this reduce power or induce unwanted dependence across genes, but it can also introduce sources of spurious signal to many genes. This phenomenon is true even for well-designed, randomized studies. We introduce "surrogate variable analysis" (SVA) to overcome the problems caused by heterogeneity in expression studies. SVA can be applied in conjunction with standard analysis techniques to accurately capture the relationship between expression and any modeled variables of interest. We apply SVA to disease class, time course, and genetics of gene expression studies. We show that SVA increases the biological accuracy and reproducibility of analyses in genome-wide expression studies.

摘要

已有明确证据表明,遗传、环境、人口统计学和技术因素可能对基因表达水平产生重大影响。除了感兴趣的测量变量外,由于未知、未测量或过于复杂而无法通过简单模型捕获的因素,往往还会产生信号来源。我们表明,在分析中未能纳入这些异质性来源会对研究产生广泛而有害的影响。这不仅会降低检验效能或在基因间引发不必要的依赖性,还会给许多基因引入虚假信号来源。即使对于设计良好的随机研究,这种现象也是如此。我们引入“替代变量分析”(SVA)来克服表达研究中异质性导致的问题。SVA可与标准分析技术结合使用,以准确捕捉表达与任何感兴趣的建模变量之间的关系。我们将SVA应用于疾病类别、时间进程和基因表达研究的遗传学。我们表明,SVA提高了全基因组表达研究中分析的生物学准确性和可重复性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e10b/1994707/1babdd26df99/pgen.0030161.g001.jpg

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